CA2211729A1 - 6-aryl pyrazolo[3,4-d¦pyrimidin-4-ones and compositions and methods of use thereof - Google Patents

Abstract

6-Aryl pyrazolo[3,4-d]pyrimidin-4-one derivatives, pharmaceutical compositions containing them and methods for effecting c-GMP-phosphodiesterase inhibition and for treating heart failure and/or hypertension.

Description

W096/28448 PCT~S96J03100 6-ARYL PYRAZOLO r 3,4-dl PYRIMIDIN-4-OMES
AND COMPOSITIONS AND METHODS OF USE T~REOF

BACKGROUND OF THE I ~ ENTION
(a) Field of the Invention:
The invention relates to 6-aryl pyrazolo[3,4-d]-pyrimidin-4-ones, to pharmaceutical compositions containing them and to methods for effectii~g c-GMP-phosphodiesterase inhibition, and treating heart failure and/or hypertension.

(b) Informat:Lon Disclosure Statement:
Schmidt e~ al., u.s. Pat. No. 3,~ 65,520, issued January 1~, 1965, disclose as coronary dilatina ~gents p~-razol~-[3,4-d]pyrimidines of general formula:
o l'J~ 1~ R3 R6 N N' wherein:
Rl represents a hydrogen atom or an alkyl, hydroxyalky', halogen-alkyl or oxa-alkyl radical or a cycloalkyl, cycloalkyi-alkyl, aralkyl or heterocyclylalkyl radical or an at mo.,t binuclear aryl cr heterocyclic radical;
R3 represents a hydrogen atom or a lower-alkyl radical;
R5 represents an aliphatic, cycloaliphatic, cyclo-aliphatic-aliphatic, araliphatic or heterocyclic-aliphat c radical; and R6 represents an aliphatic radical or an aralkyl or heterocyclyl-alkyl radical which may be substituted.
t The patent more specifically discloses as especialiy valuable the compounds in which Rl represents a hydrogen atom or a ~ lower-alkyl radical or a cycloalkyl radical, a hydro~y-lower-al}~
radical or haloaen-lower-alkyl radical, an oxa-lo.wer-alkyl, or ~n aryl radical which may be unsubstituted or mono-, di-, or tri-W 096/28448 PCTrUS96/03100 substituted by halogen, alkoxy, alkyl, methylenediox.~.T, trifluoromethyl, nitro, amino, or a pyridyl radical; R3 represen~s a hydrogen atom or a lower-alkyl radical; R5 represents a lower-alkyl radical or a lower-alkylamino radical; and R6 represents a lower-alkyl radical or an aralkyl radical.
Further disclosed are a series of 1-R1-3-R3-4-hydroxy-5-R6-pyrazolo[3,4-d]pyrimidines which are said to be useful as intermediates in the synthesis of final products. ~mong the intermediates specifically disclosed are 1-cyclopentyl-4-hydroxy-6-benzyl-pyrazolo[3,4-d]pyrimidine and 1-isopropyl-4-hydrcxy-6-rn-methoxybenzylpyrazolo[3,4-d]pyrimidine.
Schmidt et al., U.S. Pat. No. 3,211,731, issued October 1~, 1955, disclose as coronary dilating agents p,razol3-[3,4-d]pyrimidines of general formula:
OH

R6 ~ ~ N' wherein:
R1 represents hydrogen, an alkyl, hydrox-.--alkyl, halogen-alkyl or oxa-alkyl radical, a cyclo-alkyl, cycio-alkylalkyl, aralkyl, heterocyclyl-alkyl radical or an G' most binuc'ear aryl or heterocyclic radical;
R3 stands for hydrogen, or in the second place, for a lower-alkyl radical; and R6 represents a possibly substituted aralkyl or heterocyclylalkyl radical.
The patent more specifically discloses as especially valuable the compounds in which R1 represents a hydrogen atom or a lower-alkyl group, cycloalkyl, hydroxy-lower-alkyl, halogen-lower-alkyl, oxa-lower-alkyl, or an aryl; R3 represents a hydrogen atom or lower-alkyl and R6 a substituted or unsubstituted aralkyl.
Among the compounds specifically disclosed are 1-isopropyl-~-hydroxy-6-.3 -methoxyphenylmethyl)pyra7010[3,4-d]pyrimidine, 1-WO 96/28448 PC~nUS9CJO3~VO

cyclopentyl-4-hydroxy-6-benzylpyrazolo[3,4-d]pyrimidine, 1-iso-propyl-4-hydroxy-6-(l3-phenylethyl)pyrazolo[3,4-d]pyrimidine, and 1-isopropyl-4-hydroxy-6-(4-aminobenzyl)pyrazolo[3,4-d]pyrimidine.
Schmidt et al., U.S. Patent 3,211,732, issued October 12, 1965, disclose, as intermediates, 1-R1-3-R3-6-R6-4-hydroxy-pyrazolo[3,4-d]pyrimidines wherein:
R1 represents a hydrogen atom, a lower-alkyl radical which is unsubstituted or substituted by a hydroxy group or a lower-alkoxy group, or a cyclopentyl or cyclohexyl radical or a phenyl or phenyl lower-alkyl radical;
R3 represents a hydrogen atom or a lower-alkyl radical;
and R6 stands for a substituted or unsubstituted phenyl lower-al~yl radical.
Specifically disclosed is 1-isopropyl-4-hydroxy-6-benzylpyrazolo[3,4-d]pyrimidine.
Also disclosed, as intermediates, are 1-Rl-3-R3-6-R6-4-hydroxypyrazolo[3,4-d]pyrimidines wherein:
R1 stands ior a hydrogen atom, a lower-alkoxy-lower-alkyl radical or a hydroxy-lower-alkyl radical, a cyclopentyl or cyclohexyl radical or a phenyl or phenyl-lower-alkyl radical which may be substituted;
R3 has the meanings given above; and R6 stands for a phenyl radical which may be substituted.
Specifically disclosed is 1-isopropyl-4-hydroxy-5-phenylpyrazolo-[3,4-d]pyrimidine.
Breuer et al., U.S. Pat. No. 3,732,225, issued May 8, 1973, disclose as hypoglycemic agents and anti-inflammatory agents pyrazolo[3,4-d]pyrimidines of formula:
OR

R2 ~ ~ N~

W 096/28448 PCTrUS96/03100 wherein:
R is hydrogen or lower-alkyl; xl is lower-alkyl, cycloalkyl, phenyl or substituted phenyl; R2 is phenyl, substituted phenyl or cycloalkyl; and R3 is hydrogen, lower-alkyl, cycloalkyl, phenyl or substituted phenyl. Specifically disclosed are l-methyl-6-phenyl and 1-methyl-6-(4-chlorophenyl)pyrazolo[3,4-d]pyrimidin-4-ones.
British Patent 937,722, published September 25, 1963, to CIBA LIMITED, discloses as a coronary dilating agent l-isopropyl-4-hydroxy-6-benzyl-pyrazolo[3,4-d]pyrimidine.
Hamilton, U.S. Pat. No. 4,666,908, issued May 19, 1987, discloses pyrazolo[4,3-d]pyrimidine-7-ones of formula:
o HN ~ N/R

Ar-(cH2)n ~ ~ N

wherein:
R~ is lower-alkyl of from one to six carbons, inclusive, lower-alkylene of from one to six carbon, inclusive, lower-hydroxyalkyl of from one to six carbons, inclusive, lower-hydroxyalkylene of from tWO to SiY. carbons, inclusive, lower-aminoalkyl of from one to SiX carbons, inclusive, or lower-aminoalkylene of from two tO Six carbons, inclusive n is 0-4i and Ar is R2:

R2= ~(~) or 2, 3 or 4-pyridyl wherein X, Y and Z are independently (1) hydrogen; (2) lower-alkyl of from one to six carbons, inclusive;
(3) halogen; (4) hydroxyl; (5) lower-alkox.y of ~rom one tO SiX

W 096128448 PCTnUS9610310a carbons, inclusive; ~6) nitro; (7) amino; (8) NR'~" wherein R~ and RN are each independently (a) hydrogen or (b) lower-alkyl of from one to six carbons, inclusive, optionally substituted by (i) amino, (ii) morpholino, or (iii) cycloalkyl of from five to seven carbons, inclusive, ~9) sulfonyl or (10) -S02 NR'R" wherein R' and RN are as defined above.
The patent: more specifically discioses as preferred compounds those wherein Ar is R2. The compounds a-e stated to be useful in the treatment of cardiovascular disorders.
Miyashita et al., Heterocycles 1990, ~1, 1309-1314, describe the preparation of a series of pyrazol~[3,4-d]pyrimidines of general formula:
o HN

R

wherein:
R is phenyl or methyli and R1 is hydrogen, methyl, ethyl, propyl, isopropyl, benzyl, ethyl carbo~ylate or phenyl. No indication of utility is disclosed.
Hamil_~n, PCT Applicarion ~70 ~'001-2, published January 14, 1 88, discloses a series ~f 5-substituted pyrazolo[4,3-d]pyrimidin-7-one derivatives which are stated to be useful as cardio~onic, CNS stimulative, antiallergy, antiasthma or cognition activa~ing agents.
Bell et al., European Patent Applica~ion 0463755, published January 2, 1992, disclose a series of 5-(2,5-disubstituted-p:nenyl)pyrazolo[4,3-d]pyrimidin-7-ones which are stated to be use_ul in the treatment of cardiovascular disorders.
Podesva et al., U.S. patent 3,7/2,2g4, issued November 13, 19.3, disclose a process for preparing compounds of the formula I:

W 096/28448 PCTrUS96103100 Rl~ N ' H
I

wherein:
X represents a halogen atom, a free or substituted hydroxyl, amino or mercapto group and R represents a hydrogen atom, or a lower-alkyl or a substituted or unsubstituted aryl radical. The compounds are disclosed as being potentially useful in the treatment of hyperuricemia associated with gout and other conditions and additionally, the compounds wherein X represents a halogen atom are said to be useful as intermediates in the synthesis of other compounds having the formula I. Specifically disclosed is 4-hydroxy-6-phenyl-1-pyrazolo[3,4-d]pyrimidine.
Coates and Rawlings, U.S. Patent 5,075,310, issued December 24, 1991 from application Serial No. 370,494 filed June 23, 1989, disclose and claim compounds of the formula:

HN J '~
A ) ~N
(~OR1 and pharmaceutically acceptable salts thereof, wherein:

\~ .

W O 96/28448 PCTnUS96J03100 is a ring of sub-forrnula (a), (b) or ~c):

~N ~5~1 ~N

(a) (b) (c) X is oxygen or sulphur; and R1 is Cl-C6 alkyl, C2--6 alkenyl, C3-5 cycloalkyl-C1-4 alkyl, or C1-4 alkyl substituted by 1 to 6 fluoro groups. Specifically disclosed is 6 - ( 2 -propoxypheny l ) pyra zo lo [ 3, 4 -d ] pyrimidin- 4 ( 5H)- one . The compounds are said to be useful as bronchodilators and vasodi lators .
Bacon et al, U. S . Patent 5, 294, 61~ issued March 15, 1994 from Application Serial No. 859,770 filed March 30, 1992, discloses a series of 6-heterocyclyl-pyrazolo[3, 4-d]pyrimidin-4-ones, e.g., 1-cyclopentyl-3-ethyl-6- (3-pyridyl)pyrazolo[3, 4-d]pyrimidin-4-one.
The compounds are disclosed to be useful in treating heart failure and hypertension.

SU~IARY OF THE INVENTION

The invention relates to compounds of the Formula I:
o HN/~ R3 R6/ N N' I

wherein:
Rl is tert-butyl, or cyclopentyl;
R3 is lower-alkyl, or phenyl- lot~7er-alkyl i and R6 is phenyl, or phenyl substituted by from one to three, the same or different, substituents selected from the group consisting of lower-alkoxy, lower-alkyl, hydroxy, 1-imida~olyl, W 096/28448 PCT~US96/03100 lower-alkenyloxy, dilower-alkylamino-lower-alkoxy, 4-morpholinyl-lower-alkoxy, lower-alkoxycarbonyl-lower-alkoxy, carboxylower-alkoxy, trifluoromethyl, 1-piperidinyl-lower-alkoxy, 1-pyrrolidinyl-lower-alkoxy, nitro, halo, amino, -(CH2)20-, lower-alkylsulfonylamino, lower-alkoxy-lower-alkoxy, lower-alkenyl, dilower-alkylamino, -OCH(CH3)CH2-, 4-morpholinylcarbonyl-lower-alkoxy, 4-thiomorpholinyl-lower-alkoxy, pyridinyl-lower-alkoxy, 1-lower-alkyl-3-hexahydroazepinyloxy, and 1-lower-alkyl-4-piperidinyl oxy; or a pharmaceutically acceptable acid-addition salt and/or hydrate thereof.
The compounds of the Formula I have been found to possess c-GmP-PDE V inhibitory activity and are thus useful in the treatment of heart failure and/or hypertension.
Particularly preferred compounds of Formula I above are those wherein:
R1 is cyclopentyli R3 is methyl, or ethyl; and R6 is phenyl, or phenyl substituted by rrom one to two, the same or different, substituents selected from the group consisting of methoxy, ethoxy, propoxy, methvl, hydroxy, 1-imidazolyl, CH2=CHCH20-, 2-(dimethylamino)ethoxy, 3-(dimethylamino)propoxy, 2-(4-morpholinyl)e~hoxy, 3-(4-morpholinyl)propoxy, ethoxycarbonyl methoxy, arboxymethoxy, trifluoromethyl, 2-(1-piperidinyl,ethoxy, 2-(1-pyrrolidinyl)ethoxy, nitro, chloro, amino, -(CH2)20-, methylsulfonylamino, 2-(methoxy)ethoxy, CH2=CH2CH~-, diethylamino, -OCH(CH3)CH2-~ 4-morpholinyl-carbonylme~hoxy, 2-(4-thiomorpholinyl) ethoxy, 4-pyridinylmethoxy, 1-methyl-3-hexahydroazepinyloxy, and 1-methyl-4-piperidinylox~r.
Particularly preferred species of the invention are:
1- cyclopentyl-3-ethyl-6-(2-propoxyphenyl!pyrazolo[3,4-d]
pyrimindin-4-one, 1-cyclopentyl-3-ethyl-6-[4-(1-imidazolyl)phenyl]pyrazolo [3,4-d]pyrimindin-4-one, 1-cyclopentyl-3-ethyl-5-[3-(2-(4-morpholinyl)ethoxy) phenyl]pyra 7 olo[3,4-d]pyrimindin-4-one, _ W 096128448 PCT~US96103100 1-cyclopentyl-3-ethyl-6-[2-ethoxy-4-(1-imidazolyl)phenyl]
pyrazolo[3,4-d]pyrimindin-4-one, and 1-cyclopentyl--3-ethyl-6-[2-(CH2=CHCH20)phenyl]pyrazolo [3,4-d] pyrimin~in-4-one.
The invention further relates to pharmaceutical compositions which co.nprise compounds of Formula I together with a pharmaceutically acceptable carrier, adjuvant, diluent, or vehicle.
The invention further relates to a method for effecting cGMP-phosphodiesterace inhibition in a mammalian organism which comprises administering to said organism an effective amount of a compound of Formula I.
The invention further relates to a methcd for treating heart failure and/or hypertension in a mammalian ~rganism which comprises administering to said organism an effective amount of a compound of the Formula I.

DETAILED DESCRIPTION INCLUSI~JE OF PREFERRED EM~ODIMENTS
The compounds of Formula I may exist in tautomeric equilibrium with the corresponding enol form:
OH
I R~

R6/~3\ N' While the compounds are believed to be predominantly in the keto form and will be represented as such throughout this specification, it is to be understood that the invention contemplates both forms and mixtures thereof.
The term lower-alkyl as used herein means linear or branched hydrocarbon chains having from one to about four carbon atoms and thus includes methyl, ethyl, propyl, isopropyl, n-butyl, ~ sec-butyl, and the like.
The term lower-alkoxy as used herein means linear or branched alkyloxy substituents havin~ from one to about four _g _ W 096128448 PCTrUS96/03100 carbon atoms and thus includes methoxy, ethoxy, propoxy, isopropoxy, butoxy, sec-butoxy, and the like.
The term halogen, halide, or halo as used herein means bromine, chlorine, iodine or fluorine.
The term lower-alkenyl as used herein means branched or unbranched unsaturated hydrocarbon radicals of from two to about four carbon atoms and thus includes l-ethenyl, 1-propenyl, 2-propenyl, 1-methyl-2-propenyl, isopropenyl, 2-butenyl, isobutenyl, and the like.
The synthesis of compounds of the invention may be outlined as shown in Scheme A:

Scheme A

O O

R3 ~ N ~1 ~ R3 Il I

A suitably substituted 5-amino-lH-pyrazolo-4-carbcxamide ~I) is reacted with an excess of an appropriately substituted aldehyde of the formula III, optionally in the presence of a suitable organic solvent, preferably xylenes, or benzene, with or without the use of an acid catalyst, preferably p-toluenesulfonic acid, acetic acid, or methanesulfonic acid, optionally in the presence of palladium on carbon, at a temperature in the range of about room temperature up to the boiling point of the reaction mixture, preferably at the boiling point of the reaction mixture, to afford the compounds of the formula I.
Alternatively, a suitably substituted 5-amino-lH-pyrazole-4-carboxamide (II) is treated with an excess of an ester of the formula IV: R6C(O)OR wherein R is lower-alkyl, preferably ethyl, -n the presence of a base, preferably sodium ethoxiae, in W096/28448 PCT~S96103100 an alcoholic solvent, such as ethanol, at a temperature in the range of about room temperature up to the boiling point of the solvent used, preferably at the boiling point of the solvent used, to afford the compounds of the formula I.
The compou:nds of the formula I can also be synthesized as shown in Scheme B:
-Scheme B

H ~ ~ N N

Il R1 Il Vl A sui,ably substituted 5-amino-lH-pyrazole-~-carboxamide of the formu;a II is treated with an excess of a nitrile of the formula V
in a suitable organic solvent, preferably dimethylformamide (DMF), or dioxane, in the presence of an excess of a suitable base, preferably sodium hydride, at a temperature in the range of about room emperature up to the boiling point of the solvent used, to afford either the compounds of the formula I directly, or a mixture of the compounds cf the formula I and the pyrazolo[3,4-d]pyrimidin-4-amines of the formula VI. This mixture can in turn be treated with an excess of sodium nitrite, in a l/l water/acid mixtu-e, preferably a l/l water/sulfuric acid mixture, at a temperature in the range of about -10~C up to about room temperature to afford the compounds of the formula I.
Simple chemical transformations which are conventional and well known to those skilled in the art of chemistry can be used for effecting changes in the fuctional groups of the compounds of the formula I. For example, dealkylation of aryl ethe-s _o afford the corresponding phenol derivatives, hydrolysis of es_ers to afford the ccrresponding acids, catalyti_ reduction W 096/28448 PCTrUS96/03100 of nitro derivatives to afford the corresponding amines, and sulfonylation of amines to afford the corresponding sulfonamide derivatives.
The compounds of Formula I are useful both in the free base form and in the form of acid-addition salts, and, both forms are within the purview of the invention. The acid-addition salts are often a more convenient form for use; and in practice, use of the salt form inherently amounts to use of the base form. The acids which can be used to prepare the acid-addition salts include preferably those which produce, when combined with the free base, pharmaceutically-acceptable salts, that is, salts whose anions are relatively innocuous to the animal organism in pharmaceutical doses of the salts, so that the beneficial ~operties inherent in the free base are not vitiated by side effeccs ascribable to the anions. In practicing the present invention it is convenient to use the free base form or the hydrochloride, fumarate, toluenesulfonate, methanesulfonate or maleate salts. However, other appropriate pharmaceutically acceptable salts within the scope of the invention are those derived from other mineral acids and organic acids. The acid-addition salts of the basic compounds are prepared by standard procedures well known in the art which include, but are not limited thereto, dissolvina the free base in an aqueous alcohol solution containing the appropriate acid and isolating the salt by evaporating the soluticn, or by reacting the free base and an acid in an organic solven~, in which case the salt separates directly, or is precipitated with a second organic solvent, or can be obtained by concentration of the solution.
Although medicinally acceptable salts of the basic compounds are preferred, all acid-addition salts are within the scope of the present invention. All acid-addition salts are useful as sources of the free base form even if the particular salt per se is desired only as an intermediate product, as, for example, when the salt is formed for purposes of purification or identification, or when it is used as an intermediate in preparing a medicinally acceptable salt by, for example, ion exchange procedures.
The appropriately substituted 5-amino-lH-pyra701e-4-carboxamides of the formula II are either ~no~:n and thus can be W096l28448 PCT~S96~03~00 prepared by known procedures (see, for example, U.S. Patent 5,294,612, issued March 15, 1994, the entire contents of which is incorporated herein by reference), or they can be prepared by the procedures described hereinbelow in the examples. The aldehydes of the formula III, the esters of the formula IV and the nitriles of the formula V are eit:her commercially available, or they can be prepared by procedures known in the art, or by the procedures described hereinbelow in the examples.
The structures of the compounds of the invention were established by the mode of synthesis, and by one or more of elemental analysis, and infrared, nuclear magnetic resonance and mass spectroscopy. The course of the reactions and the icentity and homogenity of the products were assessed by one or more of thin layer chromatography (TLC), high pressure liquid chromatography (HPLC), or gas-liquid chromatography (GLC).
The following examples will further illustrate the invention without, however, limiting it thereto. All melting points (m.p.) are given in degrees centigrade ( C) and are uncorrected.

W 096/28448 PCTrUS961031~0 Exam~le 1 (a) A solution of salicylaldehyde (12.21 g, 0.1 mol) in DMF
(65 ml) was cooled in an ice/water bath under argon and 60% sodium hydride in mineral oil (4.0 g, 0.1 mol) was added in several portions. The mixture was stirred for one hour and then iodopropane (16.99 g, 0.1 mol) was added at room temperature. The reaction mixture was stirred at room temperature overnight, poured into water (800 ml) and stirred. The mixture was extrac~ed with chloroform (3X), the chloroform layer was concentrated in vacuo and the dark oil thus obtained was distilled under vacuum (92-94~C
at 1.15 mm Hg) to afford 12.68 g (77 %) of 2-~ro~oxvben7aldehvde.
(b) A solution of KOH (12.16 g, 184.2 mmol) in water '150 ml) was cooled in an ice-bath and then 1-cyclopentyl-3-methyl-5-amino-lH-pyrazole-4-carbonitrite (5.0 g, 26.3 mmol), followed by 30%
hydrogen peroxide (13.5 ml, 131.6 mmol) were added. The reaction mixture was warmed to room temperature and stirred overnight. A
precipitate formed which was collected by filtration and washed with ether to afford 1-cvcloDentYl-3-methvl-5-amino-lH-~vrazole-4-carboxamide, as a white solid. Additional product was obtained by concentration of the filtrate and collection of the product by filtration to afford a total of 4.46 g of product.
ilternatively, the carboxamide was prepared as fcilo..s: .
solut on of concentrated sulfuric acid (50 rnl) was cooled t-' -5~C
and 1-cyclopentyl-3-methyl-5-amino-lH-pyrazole-4-carbonitrile ~.0 g, 10.5 mmol! was added. The mixture was stirred as such tor hours, then at room temperature overnight. The reaction m xture was poured into 400 ml of ice and NH40H (100 ml) and was srirred for 1 hour. The product precipitated and was collected by filtration. Additional product was obtained by acidifyin the filtrate with acetic acid to a pH of 5 and then extracting with chloroform. The chloroform layers were concentrated in vacu and titurated with ether to afford, afte- filtration and drying at 100~C overnight, 1.67 g (76%) of 1-cvclo~entvl-3-methvl-5-a~ino-lH-~vra701e-4-carboxamide, m.p. 191-19~~C.

W ~96/28448 PCTnUS96~03100 ~ (c) A mixture of 1-cyclopentyl-3-methyl-5-amino-lH-pyrazole-4-carboxamide (3.98 g, 0.019 mol), 2-propoxybenzaldehyde (6.35 g, 0.038 mol), xylenes ~'150 ml) and methanesulfonic acid (0.5 ml) was heated at reflux for 39 hours with azeotropic removal of water.
The reaction mixture was concentrated in vacuo and the residue was treated with 10% K2CO3 and ether. The layers were separated, the aqueous layer was extracted with ether and the combined ether layers were concentrated in vacuo. Analysis of the reaction mixture by TLC indicated that the reaction was not yet complete, therefore, the mixture was heated at 180~C on an oil bath. The residue was dissolved in chloroform, and purified by column chromatography on silica gel eluting with hexane t100%) followed by ether (100%) to a~ford 2.67 g (41%) of 1-cYclo~entvl-3-methvl-6-(2-~ro~oxv~henvl)-~vrazolo~3,4-dl~vrimidin-4-one, m.p. 130-132~C
Alternatively, the final product was prepared as follows:
A mixture of 1-cyclopentyl-3-methyl-5-amino-lH-pyrazole-4-carboxamide (1.0 g, 4.8 mmol) and 2-propoxybenzaldehyde (10.6 g, 10 mmol) was heated at 160~C on an oil bath for 4 hours then at 170~C for 48 hours. The reaction mixture was cooled, chloroform (5 ml) was added and the solution was eluted on a silica gel column with ether (100 %) to afford, after recrystallization from cyclohexane, 0.16 g of 1-cvclo~entvl-3-methvl-6-(2-~ro~oxv~henvl)-~vrazolo~3,4-dl ~vrimidin-4-one.
Exam~le 2 A mixture of 1-cyclopentyl-3-ethyl-5-(4-quinolinyl-CH=N-) lH-pyrazole-4-carboxamide (6.34 g, 0.018 mol), benzaldehyde (0.96 g, 0.009 mol), xylenes (150 ml) and methanesulfonic acid (0.5 ml) was refluxed overnight. The reaction mixture was concentrated in vacuo, and the residue was treated with ethanol (200 ml) and azeotroped. The residue was then treated with 10% ~2CO3 (100 ml), titurated with ether, filtered and washed with water. The product was recrystallized from ethyl acetate and dried at 100~C to afford 2.68 g of crude product which was purified by column chromatography on silica gel to afford 0.603 g of 1-cvclo~entvl-3-ethvl-6-~henvl-~vra7Olo~3,4-dl~vrimidin-~-one, m.p. 221-222~C.

W O 96/28448 PCTrUS96/03100 Alternatively, and preferably, the final product can be prepared from 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide and benzaldehyde following a procedure similar to that described in example 1 (c).
Exam~le 3 A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (2.0 g, 9 mmol), o-tolualdehyde (2.16 g, 18 mmol), methanesulfonic acid (0.5 ml) and xylenes (50 ml) was refluxed for 32 hours. The solvent was removed and the residue was treated with ethanol (100 ml) and then concentrated to dryness. The dark residue was treated with 10% K2CO3 and chloroform, the organic layer was separated and the aqueous layer was extracted with chloroform (2 x 100 ml). The organic layers were combined, concentrated to approximately 20 ml and then added to silica gel 30 g). The preloaded silica gel was placed on a silica gel column and eluted with Et2O/hexanes (2/8) to (5/5) to afford, after drying at 70~C in vacuo, 1.10 g (40%) of 1-cvclocentvl-3-ethvl-6-(2-methvlchenvl)-cvrazolor3,4-dl~vrimidin-4-one, m.p. 133-134~C.
Examole 4 A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (2.0 g, 9 mmoli, o-ethoxybenzaldehyde (7.7 g, 18 mmol), methanesulfonic acid (5 drops), and xylenes (50 ml) was refluxed for 48 hours. The reaction mixture was stripped to dryness, and treated with 10% K2CO3 and CHCl3 (100 ml). The layers were separated and the aqueous layer was extracted with chloroform (2 x 100 ml). The organic layers were combined, and concentrated in vacuo. The dark oil thus obtained was dissol~ed in CH2Cl2 (30 ml) and combined with silica gel (30 g). The preloaded silica gel was placed on a silica gel column and eluted ~.ith Et20/hexanes (20/80) to Et20 (100%) to afford 1.41 g (45%) of 1-cvcloDentvl-3-ethvl-6-(2-ethoxv~henvl)-cvrazolor3,4-dlcvrimidin-4-one, m.p. 146-147~C.

Examcle 5 A mixture of 1-cyclopentyl-3-ethyl-5-aminc-lH-pyra7O1e-4-carboxamide (2.0 g, ? mmol), anisaldehyde (2.'5 g, 18 mmol), xylenes (50 ml) and p-~oluenesulfonic acid (0.5 g) was refluxed W096l28448 PCT~S96)031~0 for 32 hours. The reaction mixture was stripped to dryness, treated with ethanol (100 ml) and then again concentrated to dryness. The residue was treated with CHC13 (100 ml' and 10% K2CO3 (100 ml), the layers were separated and the aqueous layer was extracted with chloroform (3 x 100 ml). The com~ined organic layers were concentrated to approximately 25 ml ana then combined with silica gel (30 g). The preloaded silica ~-as placed on a silica gel column and eluted with ether/hexanes (8/10) to ether (100~) to afford 1.25 g (41%) of 1-cvclo~entvl-3-ethvl-6-(2-methoxv~henvl)-~vrazolo~3,4-dl~vrimidin-4-one, m.p. 135-136~C, after recrystalli_ation from cyclohexane.
Exam~le 6 A mixture of l-cyclopentyl-3-ethyl-5-aminc-lH-pyrazole-4-carboxamide (1.0 g, 4.5 mmol), 2-propoxybenzalder.vde (1.5 g, 9 mmol), p-toluenesulfonic acid (0.5 g) and xylenes (50 ml) was refluxed for 20 hours. The reaction mixture was stripped to dryness, treated with ethanol and again concentrated to dryness.
The residue was treated with CHC13 (100 ml) and washed with saturated NaHCO3. The organic layer was concentrated to a dark oil which was dissolved in C~2C12 (30 ml) and combined -ith silica gel (50 g). The preloaded silica gel was placed on a siiica gel column and eluted with 10% hexanes/ether to ether (100%) t~ afford, after crystallization from hexanes, 0.492 g (30 ~) of 1-c~clo~entvl-3-ethvl-6-(2-~ro~oxv~hen~ -~vrazolo~3,4-dl~vrimidin---one, m.p. 93-94~C.
Exam~le 7 To a solution of l-cyclopentyl-3-ethyl-6-(2-methoxyphenyl)-pyrazolo[3,4-d]pyrimidin-4-one (O.5 g, 1.5 mmol) in DMF (10 ml) was added NaH (0.15 g, 3.75 mmol, 60% NaH in mineral oil). The reaction mixture was stirred for 20 minutes, then propanethiol (0.228 g, 3.0 mmol) was added and the mixture was stirred at room temperature for 4 hours, then at 110~C for 9 hours. The reaction mixture was stripped to dryness and then water (15 ml) followed by a~etic acid (1 ml) were added. .~ precipitate formed which was collected by filtration, washed with water and recrystalli-~ed b. D~RCO~ treatment from ethyl acetate to afford 0.28 g (58%) _- '-c~~lo~ent~ th~ -h~rdrs~v~he~vl)-W 096/28448 PCTrUS96103100 ~vrazolo~3,4-dl~vrimidin-4-one, m.p. 272-273~C, as white fibrous needles.
Exam~le 8 (a) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (1.18 g, 5.32 mmol), 4-(1-imidazolyl)benzaldehyde (1.37 g) and xylenes (8 ml) was warmed to 130~C for 30 minutes, then to 160~C for three days. The reaction mixture was cooled, and the product was collected by filtration and washed with Et2O to afford 1.88 g of 1-cyclopentyl-3-ethyl-6-[4-(1-imidazolyl)phenyl]
pyrazolo [3,4-d]pyrimidin-4-one as the 6,7-saturated derivative.
This derivative was mixed with ethanol (300 ml) and 30% H2~2 (3.0 ml) and refluxed overnight. ~dditional 30% H2~2 (3 ml) was added and the mixture was refluxed for 8 hours. An additional 10 ml of 30% H2~2 was added and the mixture was refluxed overnight.
Starting material was still present so an additional 10 ml of 30%
H2~2 was added and the mixture was refluxed for 4 hours and then additional 30% H2~2 (10 ml) was added and the mixture was stirred for 1 hour, then was allowed to stand at room temperature overnight. The reaction mixture was stripped to a yellow liquid and purified by column chromatography on silica gel eluting with ethyl acetate (100%), then 5% methanol/ethyl acetate to afford 0.4 g of 1-cvclo~entvl-3-ethYl-6-~4-(1-imidazolvl)~henYll-~vrazolo~3,4-dl ~vrimidin-4-one 1/2 hvdrate, m.p. .- 300~C.
(b) Alternatively, the product can be obtained as follows:
To a mixture of imidazole (5.13 g, 75.35 mmol), ~2CO3 (11.45 g' and DMSO (50 ml) at room temperature was added to 4-fluorobenzonitrile (10.04 g) in one portion. The reaction mixture was stirred a~ room temperature for 1 hour, and then was warmed on a steam for 2 hours. The reaction mixture was cooled to room temperature, and poured into cold water. A precipitate formed which was collected by filtration and washed with water and recrystallized from CHC13/hexane to afford 4.07 g of 4-(1-imidazolyl)benzonitrile, m.p. 146-148~C.
~ o a mixture of 4-(1-imidazolyl)benzonitrile (0.9 g, 5.27 mmol), l-cyclopentyl-3-ethyl-5-amino-lH-PYraZole-4-carboxamide W096/28448 PCT~S96~03~

(1.17 g) in DMF (20 n~1) at room temperature was added NaH (0.63 g, 60% dispersion in mineral oil). The reaction mixture was stirred at room temperature overnight, additional NaH (0.5 g) was added and the mixture was ,tirred at room temperature for about 2 days.
The reaction mixture was poured into ice/water (500 ml), neutralized with acetic acid and the precipitate which formed was collected by filtration, washed with hexanes, dissolved in CHCl3, dried over MgSO4, fi:Ltered and concentrated in vacuo. The residue was recrystallized from ethyl acetate, combined with the product obtained from two similar experimental runs and then recrystallized from CH3CN/CHC13 to afford 1-cyclo~entvl-3-ethyl-6-~4-(1-imidazolvl)~henvl1~vrazole~3,4-dl~vrimidin-4-one, m.p.
~300~C.
Exam~le g (a) To a solution of ethyl salicylate (100 g, 0.602 mol) in DMF (400 ml) was adcled K2CO3 (150 g), followed by the dropwise addition of allyl bromide (87.5 g, 0.723 mol). The reaction mixture was then heated on a steam bath for 2 hours, the K2CO3 was removed by filtration and the reaction mixture was poured into water and extracted with ethyl acetate (3 x 300 ml). The organic layer was washed with brine, and dried over MgSO4, and the solvent was removed to afford 122 g (98%) of ethvl 2-(2-~ro~envloxv)benzoate.
(b) Sodium spheres (207 mg) was dissolved in ethanol (15 ml) and 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-CarboXamide (1 g, 45 mmol) was added, followed by ethyl 2-(2-propenyloxy)benzoate (1.85 g, 9 mmol). The reaction mixture was refluxed overnight, cooled, the ethanol was stripped and water was added. The pH was adjusted to about 7 and a solid was isolated by filtration. The solid was taken up in ether, washed with dilute HC1, dried over MgSO4, filtered and the solvent was removed and the solid residue was recrvstallized from ether to afford 0.56 g of 1-cvclo~ent~1-3-ethvl-6-r2-(CH~=CH-CH~O)~hen~ Yrazolo~3,4-dl~vrimidin-4-one, m.p. 119-120~C.
E~am~le lQ

W 096/28448 PCT~US96/03100 A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (2.03 g, 9.14 mmol), 4-[3-(dimethylamino)propoxy]
benzaldehyde (2.76 ml), and xylenes was heated at 120~C for 1 hour, then at 160~C for 6 hours. p-Toluenesulfonic acid (300 mg) was added and the mixture was heated at 160~C until the reaction was complete. The reaction mixture was cooled to room temperature, and a creamy white solid formed, which was collected by filtration, washed with methanol and recrystallized from ethyl acetate to afford 1-cvclo~entvl-3-eth~1-6- r 4- r 3-(dimethvlamino)~ro~oxvl~henvll ~vrazolor3,4-dl~vrimidin-4-one, as a white solid, m.p. 175-178~C.
Exam~le 11 (a) To a solution of salicylaldehyde ~ ml) in acetonitrile (20 ml) was added K2CO3 (5.71 g), followed by N-(2-chloroethyl)morpholine hydrochloride (3.5 g) and then the mixture was stirred at room temperature for 2 hours, then at reflux overnight. The reaction mixture was cooled to room temperature, filtered, and the filtrate was concentrated in vacuo to afford 2-r2-(4-mor~holinvl)ethoxvlbenzaldehvde, as a yellow oil.
(b) + (c) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (0.95 g, 4.28 mmol), 2-[2-(4-morpholinyl)ethoxy]
benzaldehyde (1.51 g) and xylenes (15 ml) was heated to 120~C for 1 hour, then ~o 160~C until the reaction was complete. The reaction mixture was then cooled to room temperature, the solvent was removed in vacuo, and the residue was purified by silica gel chromatography eluting with ethyl acetate (100%), followed by ethanol/ethyl acetate (1/1) to afford 1-cvclo~entvl-3-ethvl-6- r2-r2-(4-mor~holinvl~ethoxvl~henvll~vrazolor3,4-dl~vrimidin-4-one (Example ll (b)), as an oil. The free base was then converted into its hydrochloride salt, which was recrystalli~ed from ethanol and dried at 110~C under high vacuum to afford 0.5 g of 1-cvclo~entvl-3-ethvl-6-r~-r2-(4-mor~holinvl)ethoxvl~henvll~razolo r 3,4-dl pvrimidin-4-one monohvdrochloride, as an off-white powder, m.p.
235-~37~C, labelled as Example 11 (c).
Example 12 -~0-W096/28448 PCT~S96J03100 (a) A mixture of 2-formylphenoxyacetic acid t3.01 g, 0.05 mol), ethanol (4.6 g), concentrated H2SO4 (0.4 ml! and toluene (40 ml) was heated to reflux with azeotropic removai ~f water for 1 hour. The reaction mixture was poured into 10% KHCO3 (100 ml), the layers were separated and the aqueous layer was extracted with ether (2 x 75 ml). The organic layers were combined, and concentrated in vacuo to afford 9.1 g ~5 %) of 2-(ethoxvcarbonvlmethox~)benzaldehYde.
(b) A mixture of 1-cyclopentyl-3-ethyl-5-amir.~-lH-pyrazole-4-carboxamide (5.26 g, 23.7 mmol), ~-(ethoxyc~rbonylmethoxy) benzaldehyde !9.10 g, 47.3 mmol), p-toluenesulfc~ c acid ~0.2 g) and ~ylenes '100 ml) was reflu;~ed for 18 hours wi_ .he azeotropic removal cf ~;ater. The solvent was removed ir. :acuo, and the residue was .~eated with ethanol and evaporated ~o dryness. The residue was partitioned between chloroform and lC% aqueous K2CO3, the layers were separated and the aqueous layer was extracted with chloroform (100 ml). The organic layers were combined, and concentrated to dryness. The residue was preloaded on silica gel and then was purified by column chromatography on silica gel eluting with hexanes (100%) to 20% ether~hexane ~ al-ford 3.74 g (38 %) OL 1~ C 1 O I~)e n t v 1 - 3 - e t h ~ 1 - 6 - f 2 -(ethoxvcarbor.~lmetho~v)nhenvll~vrazolo ~3 4-dl~ rimidin-4-one, m.p. 116-117~r.
Exam~le 13 (a) TO a solution of 3-Hydroxyben7aldehyde 3.05 g, 24.97 mmol) in acetcnitrile (15 ml) was added K~CO3 (7.6 g), followed by N-(2-chloroeth-~-l)morpholine hydrochloride (4.65 gj. The reaction mixture was s-irred at room temperature for 30 minutes, then at reflux overnight. Additional M-(2-chloroethyl)morpholine hydrochloride (0.93 g) and K2CO3 (0.7 g) were added and the mixture was refluxed for an additional 6 hours. The reaction mixture was cooled to room temperature, filtered and the filtrate was concentrated in vacuo. The residue was partitioned between water and chl~-oform, the layers were separated and the aqueous W 096/28448 PCTrUS96/03100 layer was extracted with chloroform (2 x 75 ml). The c~ganic layers were combined, washed with brine, dried over ~IgSO4, filtered and stripped to afford 7.3 g of 3- r 2-(4-mor~holinvl)ethoxvlbenzaldeh~de, as an amber liquid.
(b) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (1.05 g, 4.73 mmol), 3-[2-(4-morpholinyl)ethoxy]
benzaldehyde (1.67 g) and xylenes (7 ml) was heated to 160~C
overnight. Additional aldehyde (0.4 g) was added and the mixture was heated at 160~C until the reaction was complete. The reaction mixture was cooled to room temperature and a solid formed which was collected by filtration and washed.with ether. The f,ltrate was concentrated to dryness and the residue was combined t~ith the solid and was purified by column chromatography on silica gel eluting with ethyl acetate/ethanol (60/40). The solid produc_ thus obtained was washed with ether, recrystallized from ethyl a_etate and then washed with ether again to afford 1-oYclo~entvl-,-ethvl-6-~3-~2-(4-moroholinyl)ethoxvl~henvll-~vrazolo~3,4-dl~vrimidin-4-one, m.p. 173-176~C.
Exam~le 14 ~ mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (1.19 g, 5.38 mmol), 2-methoxy-4-carboxymethoxybenzaldehyde !1.13 g) and glacial acetic acid (25 ml) was warmed to reflux for 4 days. The reaction mixture was cooled to room temperature and the solvent was stripped to afford a slurry which was washed with methanol, collected by filtration and ~hen washed with ether. The product was recrystallized from ethanol and ~Jashed with ether to afford 1-cvclo~entvl-3-ethvl-6-~(2-me~hoxv-4-carboxvmethoxv)~henvll~vrazolo~3,4-dl~vrimidin-4-one.
Exam~le 15 ~ mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (0.59 g, 2.65 mmol), 2-trifluoromethylbenzaidehyde (0.5 mi' and glacial acetic acid (25 ml) was refluxed overnight and then 0.5 equivalents of additional aldehyde was added and the mixture was refluxed for about 3 days. The reaction mixture was cooled ~o room temperature, the acetic acid was stripped an~ the W096/28448 PCT~S96J0310~

residue was cooled and rinsed with ether to give a white solid which was collected by filtration and recrystallized from tert-butyl dimethyl etherihexanes to afford 1-cvclo~entYl-3-ethvl-~-(2-trifluoromethYl~henvl)-~vrazolo~3,4-dl~Yrimidin-4-one, m.p. 201-202 ~C.
Exam~le 16 A mixture of 1-cyclopentyl-3-ethyl-6-[2-(ethoxycarbonylmethoxy)pheny]pyrazolo[3,4-d]pyrimidin-4-one (3.0 g, 7.3 mmol), K2CO3 (3.04 g), water (20 ml) and ethanol (50 ml) was refluxed for 1.5 hours. The reaction mixture was cooled, the solvent was removed in vacuo and the residue was slurried with water and acidified. A precipitate formed which was collected by filtration, recrystallized from isopropanol and dried at 90~C. The solid was dissolved in 10% K2CO3 (100 ml), treated with DARCO~
filtered and the filtrate was acidified with acetic acid. A
precipitate formed w~ich was collected by filtration and dried at 110~C. The solid product was combined with the solid product obtained from a similar experimental run, stirred with 6N HCL (100 ml), filtered and dried with P2Os at 100~C under vacuum to afford 2.09 g of 1-cvclo~entYl-3-ethvl-6- r 2-(carboxvmethoxv)~henvll ~vrazolo~3,4-dl~vrimidin-4-one 1/2 hvdrate, m.p. 20&-209~C.
Exam~le 17 (a) To a rnixture of wa~er 500 ml) and 85% KOH 37.91 g) at 0 ~C was added 30% H2O;2 !49.4 ml, 483 mmol), followed by 1-tert-butyl-5-amino-lH-pyra;~ole-4-carbonitrile (15.83 g, 96.5 mmol). The reaction mixture was stirred for four hours at 0~C and then at room temperature for 1 hour. ~ yellow precipitate had formed which was collected by filtration and air dried to afford 13.2 g (75%) of 1-tert-butyl-5-amino-lH-~vrazole-4-carboxamide, m.p. 193-195~C.
(b) A mixture of 2-propo.Yybenzaldehyde (3.0 g, 18.27 mmol), 1-tert-butyl-5-amino-lH-pyrazoie-4-carboxamide (2.5 g, 13.7 mmol), methanesulfonic acid (0.2 ml) and xylenes (50 ml) was refluxed overnight. The reaction mixture was stripped to dryness, treated with ethanol and again stripped to dryness. The residue was partitioned between chloroform and 10% KHCO3, the layers were -~3-W 096/28448 PCTrUS96/03100 separated, and the aqueous layer was extracted with chloroform (2 x 100 ml). The organic layers were combined, and concentrated in vacuo and the residue was dissolved in CH2Cl2 (30 ml) and combined with silica gel (20 g). The preloaded silica gel was placed on a silica gel column and eluted with 70% ether/hexanes, followed by ether (100%) to afford 0.98 g (22%) of 1-tert-butvl-6-(2-~henyl)~vrazolor3~ 4-dl~vrimidin-4-one 1/100 hvdrate, m.p.
130-131~C.

(c) A mixture of 1-tert-butyl-6-(2-propoxyphenyl)pyrazolo[3,4-d]pyrimidin-4-one lilOO hydrate (0.68 g, 2.1 mmol) and trifluoroacetic acid (50 ml) was heated on a steam bath for 3.5 hours. The reaction mixture was stripped ~o dryness and the residue was purified by column chromatography on silica gel eluting with ether to afford 0.45 g (79%) of 6-(2-~ro~oxv~henvl)~yrazolo~3~4-dlpyrimidin-4-one 1,'4 hvdrate, m.p.
170-171~C.
Exam~le 18 (a) To a solution of 4-hydroxybenzaldehyde (4.04 g, 33.08 mmol), in acetonitrile (50 ml) was added K2C03 (10.1 g), followed by N-(2-chloroethyl)morpholine hydrochloride ~6.16 g). The reaction mixture was heated to reflux overnight, additional N-(2-chloroethyl)morpholine hydrochloride (0.6 g) and ~Co3 (0.5 g) were added and the mixture was refluxed for another 3 hours. The reaction mixture was cooled to room temperature, filtered, and the filtrate was treated with DARCo~, filtered and the solvent was stripped. The residue was partitioned between saturated NaHC03 (150 ml) and ethyl acetate (300 ml). The layers were separated and the organic layer was washed with lN NaOH, dried over MgS04, filtered and stripped to afford, as an amber oil, 6.41 g of 4-~2-(4-mor~holinvl)etho~lbenzaldehvde.
(b) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (2.19 g, 9.86 mmol), 4-[2-(4-morpholinyl)ethoxy]ben7aldehyde ~3.5 g) and xvlenes (10 ml) was W O g6t28448 PCTnUS96103100 heated at 160~C overnight. p-Toluenesulfonic acia (0.2 g) was added and the mixture was heated at 160~C overnight. The reaction mixture was cooled to room temperature, and the precipitate which formed was slurried with methanol, collected by - ltration and washed with methanol, and then ether. The ~roduct was recrystallized from acetonitrile to afford 1-cvclo~e~tvl-3-ethvl-6-r4-r2-(a~-mor~holin~l)ethoxvl~henvll~vrazolo~3,4-dl~vrimidin-4-one.

Exam~le 19 (a) To a mixture of 3-hydroxybenzaldehyde -.42 g, 44.38 mmol), K2CO~ (13.5 g) and acetonitrile was ~dded N-(2-chloroethyl)piperidine hydrochloride (9.8 g). The r_~ction mixture was refluxed overnight, cooled to room temperature and filtered.
The filtrate was stripped to give an oil which ~.~as partitioned between CHC13 (350 ml) and lM NaOH (200 ml). The oraanic layer was separated, washed with lM NaOH (2 x 200 ml), treated with DARCO~, then MgSO4, filtered, and stripped to afford, as a dark oily liquid, 6.28 g of 3-~2~ ~i~erdinvl)ethoxvlbenzaldeh~de.
(b) A mix~ure of 1-cyclopentyl-3-ethyl-5-amino~ pyrazole-~-carboxamide ~2.02 g, 9.09 mmol), 3-[2~ piperi~-nyl)]ethoxy]
benzaldehyde (3.18 g) and xylenes (10 ml) was reflu.-ed overnight.
Additional aldehyde (0.5 g) was added and the mixture was heated at 160~C for ~ hours. The reaction was still not -omplete so an additional 0.5 g oi- aldehyde was added and the mixture was refluxed for about 2 days. The reaction mixture was cooled, filtered and s~ripped tO afford an oily residue. The residue was treated with acetonitrile and chilled and the precipitate which formed was ccllected by filtration and washed wi-h ether. The product was purified by column chromatography cn silica gel eluting t~Tith ethyl acetate/hexanes (1/1), followed by recrystallization from acetonitrile to afford, as a white solid, 1-cvclo~en~-.-1-3-ethvl-6-~3-~2-(1-=

W 096/28448 PCTrUS96103100 ~i~eridinvl)ethoxvl~henvll~Yrazolo~3,4-dl~rimidin-4-one, m.p.
180~C
Exam~le 20 (a) To a mixture of 3-hydroxybenzaldehyde (5.17 g, 42.34 mmol), K2C03 (5.85 g) and acetone (50 ml) was added ethyl bromoacetate (5.2 ml). The reaction mixture was stirred at room temperature overnight, additional K2C03 (1 equivalent) .~was added, the mixture was stirred for one hour, then additional ethyl bromoacetate (0.5 equivalents) was added and the mixture was stirred at room temperature until the reaction was complete. The reaction mixture was filtered, water was added to the filtrate and the solvent was removed. The residue was dissolved n ether, extracted with lM NaOH (2 x 100 ml), and the ether layer was dried over MgS04 and stripped to afford, as a liquid, 7.89 g of 3-(ethoxvcarbonvlmethoxv) benzaldehvde.
(b) A mixture of l-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (3.54 g, 15.95 mmol), 3-(ethoxycarbonylmethoxy) benzaldehyde (4.3 g) and xylenes (20 ml) was heated at 160~C
overnight. The reaction mixture was cooled to room temperature, a solid formed which was collected by filtration and .~ashed with methanol and then ether. The product was recrystalli7ed from acetonitrile to afford 2.48 g of 1-cvclo~entvl-3-ethvl-6- r3-(ethoxvcarbonvlmethoxv)~henvll~vra7olo~3,4-dl~vrimidin-4-one. ~n addit:ional 0.3 g of product was also obtained from the recrystallization of the filtrate for a total of 2.78 g.
Exam~le 21 To a slurry of l-cyclopentyl-3-ethyl-6-[3-(ethoxycarbonylmethoxy)phenyl]pyrazolo[3,4-d]pyrimidin-4-one (1.23 g, 3.0 mmol) in ethanol (10 ml) was added water (100 ml), followed by 85% KOH (0.4 g). The reaction mixture was heated on a steam bath for 3 hours, cooled to room temperature and filtered. The filtrate was chilled and acidified with acetic acid to afford a white precipitate, which was collected by filtration and washed with water, then ethanol, and finally ether. The product was combined with the product from another experimental run and then -~6-WO 96/28448 PCTnUSg6J0310~

was recrystallized from DMF/CH3CN to afford 0.98 g of 1-cvclo~entvl-3-ethvl-6-~3-(carboxvmethoxv)~henvll~vrazolo~3,4-dl~vrimidin-4-one, m.p. 299-300~C.
Exam~le 22 (a) To a mixture of 3-hydroxybenzaldehyde (4.15 g, 33.98 mmol~, KOH (4.93 g) and DMSO (50 ml) was added N-(2-chloroethyl) pyrrolidine hydrochloride (6.94 g). The reaction mixture was stirred at room temperature overnight, then was poured into water (750 ml) and ethyl acetate (350 ml) was added. The layers were separated, the aqueous layer was extracted with ethyl acetate and the combined organic layers were washed with water (2 x 1000 ml), drie~ over MgSO4, fi:Ltered and stripped to afford 7.12 g of 3-~2-(1-~.rrolidinvl)etho-~vlben7aldehvde.
(b) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazolo-4-carboxamide (2.32 g, 10.45 mmol), 3-[2-(1-pyrrolidinyl)ethoxy]
benzaldeyde (2.98 g), and xylenes (10 ml) was heated at 160~C
overnight. Additional aldehyde (0.5 g), and p-toluenesulfonic acid (0.5 g) were added and the heating was continued at 160~C
overnight. The reaction mixture was cooled, the solvent was stri?ped and the residue was purified by column chromatography on sili_a gel eluting with ethyl acetate (100%) then ethanol/ethyl acetate (1!1), followed by recrystallization of the product from acetGnitrile. Additional product was obtained by preparative thin layer chromatography of the mother liquors from the recrystallization steps eluting with ethyl acetate to afford a tota_ of 0.6 g (14 %) of 1-cvclo~entvl-3-eth~l-6-r3-r2-( ~vrr-lidinvl)ethoxyl~henvll~vrazolo~3,4-dl~vrimidin-4-one.
Exam~le 23 (a) To a mixture of 3-hydroxybenzaldehyde (5.44 g, 44.55 mmol , K2CO3 (13.6 g) and DMF (50 ml) was added in portions 2-dime~hylaminoethylchloride hydrochloride (7.1 g). The reaction mixture was stirred at room temperature overnight, filtered and the iltrate was stripped. The residue was diluted with lM HCl (30Q ml), and extracted with ether, and the ether layer was dried _~ I _ W 096/28448 PCTrUS96103100 over MgSO4 and stripped. The acidic aqueous layer was cooled and then treated with 8N NaOH till basic, then it was extracted with ether (3 x 150 ml). The ether layers were combined, dried over MgSO4, filtered and stripped to afford, as an oily liquid, 1.43 g of 3-~2-(dimethvlamino)ethoxvlbenzaldehvde.
(b) + (c) A mixture of l-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (3.50 g, 15.74 mmol), 3-[2-(dimethylamino)ethoxy]
benzaldehyde (3.95 g) and xylenes (10 ml) was heated at 160~C
overnight. The reaction mixture was cooled to room temperature, the solvent was stripped, and the residue was partitioned between chloroform and water. The layers were separated, and the aqueous layer was extracted with chloroform. The organic layers were combined, washed with brine, dried over MgSO4, filtered and stripped to afford, as an oil, l-cvclo~ent~ 3-ethvl-6-!3-~2-(dimethvlamino)ethoxvl~henvil~vrazolo~3,4-dl~vrimidin-4-one labelled as ~Example 23 (b)]. The free base was treated with ethanolic HCl to afford the product as the hydrochloride salt [labelled as Example 23 (c)].
Exam~le 24 (a) A mixture of 3-fluorobenzonitrile (18 ml, 158.38 mmol), imidazole (11.46 g), K~C03 (25.59 g), copper (1.75 g), potassium iodide (1.75 g) and DMF (125 ml) was refluxed overnight. The reaction mixture was cooled to room temperature and poured into ice/water (600 ml). ~ precipitate formed, which was collected by filtration, washed with water, dissolved in ethanol (25 ml)/CHC13 (500 ml) and filtered. The filtrates were partitioned in water, the organic layer was separated, dried over MgSO4 and stripped.
The residue was combined with the product from another experimental run and was recryscallized from CHC13/hexanes to afford 13.4 g of 3-(1-imidazol~il)benzonitrile.
(b) To a mixture of 3-(1-imidazolyl)benzonitrile (3.16 g!, 1-Cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-Carboxamide (3.,7 g, 16.98 mmol) and DMF (75 ml) was added NaH (0.78 g, 60% dispersion in mineral oil). The reaction mixture was stirred at room W O 96128448 PCTnUS96103100 temperature for about 2 days, then additional nitrile (0.1 equivalents) and NaH (0.2 equivalents) were added an~ the mixture was stirred at room temperature overnight. The solvent was stripped, and the re~sidue was partitioned between chloroform (150 ml) and water (350 ml). The layers were separated, the aqueous layer was extracted with chlorform (2 x 100 ml), and the organic layers were combined, washed with brine, dried over MgSOl, filtered and stripped. The product was dissolved in hot tert-butyldimethyl ether, filtered and stripped. The residue w~s treated with CH3CN and the solid which formed was collected by filtration to affor~. 2.10 g of 1-cvclo~entvl-3-e h~1-6-~3-(l-imidazol~l)~henvll~ra7010 ~3,4-dl~vrimidin-4-amine.
( c ) To a solution of 1-cyclopentyl-3-e~hyl-6-[3-(l-imidazolyl)phenyl]pyrazolo[3,4-d]pyrimidin-4-amine 6.24 g, 16.7 mmol), in 45 ml of H~O/H2S04 (1:1) in an EtOH/ice bath was ad~'ed sodium nitrite (5.77 g) in water (5 ml) in small por~ions over 1.5 hours. The reaction mixture was warmed to room temperature ..nd stirred overnight. T~le reaction mixture was poured :nto ice/water (500 ml) and neutralized with NH40H to afford a yell~w precipitl~e which was collected by filtration, washed with wate-, then eth~r.
The product was recrystallized from EtOAc/MeOH, -hen MeOH ro afford 1 - c v c l o ~ e n t v 1 - ~ - e t h v 1 ~ 3 - ( 1 -imidazolvl~henvl?~vra olo~3,4-dl~vrimidin-4-one, m.p. 264-265~C.
Exam~le 25 (a) To a mixture of 3,4-dihydroxybenzaldehyde !3.46 g, 25.05 mmol), K2C03 (11.08 g) and DMF (50 ml) which was s_irred at rc~m temperature for 1 hour, was added N-(2-chloroethyl)morphol~e hydrochloride (g.79 g). The reaction mixture was stirred at rc~m temperature overnight, then on a steam bath for 6 hours. Start~ng material was still present so additional K2Co3 (1./3 g) and N- 2-chloroethylimorpholine hydrochloride (~.66 g) were added and ~he mixture was heated on a steam bath overnight. The reaction mixtl:re was filtered, the fil.trate was stripped and the residue was ta-:en up in 2N HCl (200 m:L) and partitioned with CHCl3 (100 ml). The a~ueous laye- was extracted with CHC13 ~2 x 150 ml), and ~he W 096/28448 PCTrUS96/03100 organic layers were combined. The aqueous layer was chilled, t';en treated with concentrated NH40H until neutral. The aqueous layer was then extracted with CHC13 (3 x 150 ml), and the organic layers were combined, washed with brine, dried over MgSO4, filtered ,~nd stripped to afford 3,4-r2-(4-mor~holinvl)ethoxvlbenzaldehvde.
(b) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (2.09 g, 9.4 mmol), 3,4-[2-(4-morpholinyl)etho:y]
benzaldehyde (5.14 g) and xylenes (25 ml) was heated at 160~C ~or about 2 days. Starting material was still present so p-toluenesulfonic acid (6.0 g) was added and the mixture was heated at 160~C overnight. The reaction mixture was cooled to room temperature, water and methanol were added and the mixture ~as stripped tG afford an oily residue. The residue was partitio::ed between lN NaOH (300 ml) and EtOAc (100 ml), the layers t~re separated, and the aqueous layer was extracted with EtOAc (1 x .50 ml). The organic layers were combined, washed with brine, dried over MgSO4, filtered and stripped. The solid product as recrystallized from EtOAc to afford 1.51 g of 1-cvclo~entvl-3-ethY1-6-~3,4-~2-t4-mor~holinvl)ethoxvl~henvll~vrazolo~3,4-dl~vrimidin-4-one.
Exam~le 26 (a) To G mixture of ethyl 2-hydroxybenzoate (2.4 ml, 16.38 mmol) K~C53 (4.93 g), and DMF (30 ml) was added N-~3-chlort~propv'~morpholine hydrochloride (3.~3 g). The mixture ~as stirred at r~om temperature for 30 minutes, then was warmed or a steam bath overnight. The reaction mixture was cooled, filte~ed and stripped to afford a liquid which was partitioned bet~en EtOAc (350 ml) and water. The organic layer was separated, was~.ed with water '2 x 200 ml), dried over MgSO4 and stripped to aff(rd ethvl 2-~3-'~-mor~holinvl)~ro~ox~lbenzoate.
(b)+(c) Sodi~m spheres (0.42 g) were dissolved in ethanol (20 rrl) and then 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxam~de (2.02 g, ~.10 mmol) was added, followed by ethyl 2-[3-'4-morpholinyl~propoxy]benzoate (5.33 g). The reaction mixture ~as W096/28448 PCT~S96103100 refluxed for 3 days, then stirred at room temperature, and then the solvent was stripped. The residue was dissolved in water (250 ml), acidified to a pH o~ about 7 with acetic acid and extracted with CHCl3. The organic layers were washed with brine, dried over MgSO4 and stripped to afford an oil. The oil was taken up in ether, filtered and the filtrate was stripped and purified by column chromatography on silica eluting with EtOAc (100%) followed by EtOAc/MeOH (80/20) to afford 2.71 g of 1-cyclopentyl-3-ethyl-6-[2-[3-(4-morpholinyl)propoxy]phenyl]pyrazolo[3,4-d]pyrimidin-4-one, as a liquid [labelled as Example 26 (b)]. The free base wastreated with EtOH-HCl and 1.14 g of the hydrochloride salt (labelled as Example 26 ~c)) was obtained, m.p. 220-221~C.
Exam~le 27 (a) To a stirred solution of KOH (5.81 g) in DMSO (15 mL) was added imidazole (5.0 g, 73.4 mmol). The mixture was stirred for 1 hour, then 2-fluorobenzonitrile (8.76 mL) in DMSO (10 mL) was added dropwise over 20 minutes. The reaction mixture was stirred at room temperature overnight and the product was collected by filtration and washed with water to afford 10.91 g of 2-(1-imidazolvl)benzonitrile as a white solid.
(b) To a mixture of 2-(1-imidazolyl)benzonitrile (3.14 g), 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (3.,5 g, 16.59 mmol) and DMF (75 ml) was added 60% NaH (0.78 g, 60%
dispersion in mineral oil). The reaction mixture was stirred at room temperature overnight, poured into ice/water (600 ml) and treated with acetic acid until a pH of 7 was obtained. The product was collected by filtration, and recrystallized from EtOAc/hexane to afford 2.82 g of 1-cvclo~entvl-3-ethvl-6- r 2 ! 1 -imidazolvl)~henyll~vr~zolor3,4-dl~vrimidin-4-amine-1/4 hvdrate.
(c) To a solu~ion of 1-cyclopentyl-3-ethyl-6-[2-(1-imidazolyl)phenyl]pyrazolo[3,4-d~pyrimidin-4-amine 1/4 hydrate ~ (2.55 g, 6.837 mmol) in 35 ml of H20/H2SO4 (1/1) in an EtOHiice bath was added dropwise NaNO2 (2.36 g) in water (10 ml) over 2 hours. The reaction mixture was stirred ovenight, poured into ice water (750 ml) and neutralized with ~H40H. ' precipitate formed which was collected by filtration, and washed with water, then ether to afford 0.75 g of the product. An additional 1.74 g of product was extracted from the filtrate and these combined product fractions were recrystallized from EtOAc, and then were dissolved in chloroform and stripped to afford, as a white powder, 1.42 g of 1-cvclo~entvl-3-ethvl-6-~2-(1-imidazolvl)~henvll~vrazolor3,4-dl~vrimidin-4-one, m.p. 192-194~C.
Exam~le 28 A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (2.0 g, 9 mmol), 4-nitrobenzaldehyde (2.04 g, 13.5 mmol), methanesulfonic acid (0.25 ml) and xylenes (50 ml~ was heated at reflux overnight, followed by an additional 6 hours.
Ethanol (200 ml) was added to the reaction mixture, which was then refluxed and then treated with DARCO~. The reaction mixture was filtered, concentrated to 100 ml and then cooled. Yellow needles formed, which were collected by filtration and washed with ether to afford 0.53 g (17%) of 1-cvclo~ent~1-3-ethvl-6-~4-nitro~henvl)~vrazolo r 3,4-dl~yrimidin-4-one, m.p. 321-323~C (dec.).
Exam~le 29 (a) To a mixture of 1-cyclopentyl-3-ethyl-5-am1no-lH-pyrazole-4-carboxamide (5.0 g, 22.5 mmol), ethyl 4-chloro-~-ethoxybenzoate (5.4 g, 23.6 mmol) and DMF (50 ml) cooled in an ice bath was added NaH (3.9 g, 97.5 mmol, 60% dispersion in mineral oil). The reaction mixture was stirred in the ice bath for 2 hours, then at room temperature overnight. The reaction mixture was then concentrated in vacuo, and the residue was treated with water (100 ml) and acidified with acetic acid. The mixture t~as extracted with CHCl3 (2 x 150 ml), the organic layers were concentrated in vacuo and the oily residue was crystallized from ether. The product was collected by filtration and dried. Recrystallization of the product from isopropanol/ether afforded 6.2 g of l-cvclo~entvl-~-ethvl-5-(4-chloro-~-erhoxv~henvlcarboxamido)-lH-~vrazole-4-carboxamide, m.p. 1-5-177~C.
(b) -~2-CA 022ll729 l997-07-29 WO 96/28448 PCTAUS96)D31~D

A mixture of 1-cyclopentyl-3-ethyl-5-(4-chloro-2-ethox,vphenylcarboxamido)-lH-pyrazole-4-carbOxamide (1.0 g, 2.11 mmol) and N-methyl-2-pyrrolidinone (3 ml) was heated at 185 - 190~
C for 6 hours. I~he reaction mixture was cooled to room temperature, and treated with water (25 ml) and the product was collected by filtration and recrystallized from isopropanol to afford 1 -cv c lo~ e ntv 1 -3 - et hv l - 6- (4 - c h lor o -2 -ethoxv~henvl)~vrazolor3,4-dl~vrimidin-4-one, m.p. 1&5-187~C.
Exam~le 30 A mixture of 1-cyclopentyl-3-ethyl-5-(4-chloro-2-ethoxyphenylcarboxamido)-lH-pyrazole-4-carboxamice (4 g, 9.8 mmol), imidazole (5.0 g, 73.5 mmol), E~F (4.5 g, 7,.~ mmol) and N-methyl-2-pyrrolidinone (lO ml) was heated at 185 - 90 ~C for 2.5 hours, then at room temperature overnight. Water (~0 ml) was added to the reaction mixture, and the mixture was acidif-ed with acetic acid. A precipitate formed which was collected _v filtration, washed with water and dried to afford 2.8 g of 1--vclo~entvl-3-ethvl-6-(4-chloro-2-hYdroxv~henvl)~vrazolo r 3,4-dl~vrimidin-4-one, as white needles, m.p.> 300~C.
Exam~le 31 To a mixture of 1-cyclopentyl-_-ethyl-6-~4-nitrophenyl)pyrazolo[3,4-d]pyrimidin-4-one (1.38 g, 3.9 mmol), SnCl2-2H20 (2.64 g, 11.72 mmol), ethanol (24 ml) and water (10 ml) was added concentrated HCl (14.5 ml). The reacti~n mixture was refluxed for 2 hours, cooled, and the product was collected by filtration and dried in vacuo to afford 0.85 g (67%) of 1-cvclo~entv'-3-eth~l-6-~4-amino~henvl)~vrazolo~3,4-dl~vrimidin-4-one hvdrochloride 1/3 hvdrate, m.p. 279~C (dec.).
Exam~le 32 A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide '2.0 g, 9.0 mmol), 2,3-dihydroben70[b]furan-5-carboxaldehyde (1.73 g, 11.7 mmol), methanesulfonic acid (0.25 ml) and xylenes (50 ml) was refluxed for 20 hours and then allowed ~o stand for about days. The reaction mixture was diluted with ether and the product was collected by filtration and dried to afford 1.~5 g (52%) of 1-cvclo~entvl-3-ethvl-~-/2,3-W 096128448 PCTrUS96/03100 dihvdrobenzorbl furan-5-vl)~vrazolo~3,4-dl~vrimidin-4-one 1/10 hvdrate, m.p. 253-254~C.
Exam~le 33 To a mixture of 1-cyclopentyl-3-ethyl-6- (4-aminophenyl)pyrazolo[3,4-d]pyrimidin-4-one hydrochloride 1/3 hydrate (0.61 g, 1.7 mmol) in dry pyridine (20 ml) in an ice bath was added methanesulfonyl chloride (0.49 g, 4.25 mmol). The reaction mixture was stirred at room temperature for about two days, the solvent was stripped to dryness and the residue was treated with water. The product was collected by filtration and recrystallized from ethanol, after DARCO(~) treatment, to afford 0 .49 g (7 2%) o f 1 - c v c l o ~ e n t v l - 3 - e t h v 1 - ~ - r 4 (methvlsulfonvlamino)~henvll l~vra7Olo~3,4-dll~vrimidin-4-one, m.p.
325~C (dec.).

Exam~le 34 (a) To a solution of 2-hydroxybenzaldehyde (6.11 g, 0.05 mol) in DMF (50 ml) under argon in an ice bath was added NaH (2.0 g, 0.05 mol, 60% dispersion in mineral oil), followed 1 hour later by 2-chloroethylmethyl ether (4.73 g, 0.05 mol). The reaction mixture was allowed to stand for about 2 days, then was heated at 70~C for 7 hours. The reaction mixture was stripped to dryness, the residue was partitioned between water and CHCl3, the layers were separated and the aqueous layer was extracted with CHCl3 (2 x 75 ml). The product appeared to be in both layers, thus they were concentrated in vacuo and the residue was purified by column chromatography on silica gel eluting with ether to afford 1.5 g of 2 - ~2 -(methoxv)ethoxvlbenzaldehvde.
(b) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (1.07 g, 4.8 mmol), 2-[2-(methoxy)ethoxy]benzaldehyde (1.31 g, 7.2 mmol), xylenes (40 ml) and methanesulfonic acid (0.25 ml) was refluxed overnight. The reaction mixture was stripped to dryness, the residue was partitioned between CH2Cl~ and water, the layers were separated and the aqueous layer was extracted with W O 96/28448 PCTnUS96103100 CH2C12 (2 x 100 ml). The organic layers were combined, concentrated in vacllo and combined with silica gel (30 g). The preloaded silica gel was placed on a silica gel column and eluted with hexane/ether (1/1) to afford, after crystallization from hexane/tert-butylmethyl ether (25/1), 0.305 g (17%) of 1-cvclo~entvl-3-ethvl-6- r 2- r 2-(methoxv)ethoxYl~henvl l ~Yrazolo r 3,4-dl~vrimidin-4-one, m.p. 71-72 ~C.
Exam~le 35 (a) To a solutioi~ of 3-hydroxy-4-methoxybenzaldehyde (8.56 g, 56.26 mmol) in CH3CN (50 ml) was added K2CO3 (17.1 g) with CH3CN
(20 ml), followed 20 minutes later by N-(2-chloroethyl)morpholine hydrochloride (11.52 g). The reaction mixture was refluxed overnight, and then was cooled to room temperature, filtered, and the solvent was stripped to give, as an amber oil, 4-methoxv-3- r2-(4-mor~holinvl)ethoxvlben7aldehvde.
(b) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (1.25 g, 5.63 mmol), 4-methoxy-3-[2-(4-morpholinyl)ethoxy]benzaldehyde (1.64 g), and ~vlenes (12 ml) was heated at 160~C overnight. Additional aldehyde (0.5 g) was added and the mixture was refluxed until complete, then cooled to room temperature. The solvent was stripped, the residue was slurried with EtOAc and the product was collected by filtration and combined wlth the product from a similar experimental run. The combined product was recrystallized from CH3CN to afford 1-cvclo~entvl-3-ethyl-6-r4-methoxy-3-~2-(4-mor~holinvl)ethoxvlr)henvll~vrazolor3,4-dl~vrimidin-4-one, m.p.
205-206~C.
Exam~le 36 1-cyclopentyl-3-ethyl-6-[2-(CH2=CH-CH20)phenyl]pyrazolo [3,4-d]pyrimidin-4-ore (5.84 g) was heated at 210~C for 2 hours.
Ether was added and the mixture was filtered and the product was recrystallized from ethanol, then DMF to afford 3.42 g of 1-cYcio~entvl-3-ethvl-6-~2-hvdroxy-3-(2-Dro~envl)~hem~ yrazolo r3, 4-dl~yrimidin-4-one, m.p. > 280~C.
Exam~le 37 W 096128448 PCTrUS96/03100 (a) To a mixture of 2-hydroxy-4-(diethylamino)benzaldehyde (10.0 g, 51.75 mmol), K2CO3 (14.3 g) and DMF (150 ml) at room temperature was added ethyl iodide (4.1 ml). The reaction mixture was stirred for about two days, filtered and the filtrate was concentrated in vacuo. The residue was partitioned between ether and saturated Na2CO3, and the organic layer was separated, dried over MgSO4, treated with charcoal, filtered and concentrated in vacuo. The solid product was recrystallized from hexane to afford, as a pink crystalline solid, 9.8 g of 2-ethoxv-4-(diethvlamino)benzaldehvde, m.p. 58-59~C.

(b) A mixture of 2-ethoxy-4-(diethylamino)benzaldehyde (7.87 g, 35.56 mmol), 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (3.95 g, 17.78 mmol), p-toluenesulfonic acid monohydrate (0.05 g), 10% palladium on carbon (0.11 g) and benzene (150 ml) was refluxed overnight with the azeotropic removal of water. The catalyst was removed by filtration, and the filtrate was concentrated in vacuo. The residue was combined with that from a similar experimental run, and dissolved in CH2Cl2, and loaded onto a silica gel column. Elution of the column with ether/hexane (60/40) afforded a green foam which was titurated with refluxing hexane, and cooled and the product, as pale vellow needles, was collected by filtration to afford 1.19 g (8%) of 1-cvclo~entvl-3-ethvl-6-~2-ethoxv-4-(diethvlamino)~henvll~vrazolo~3~4-dl~vrimidin 4-one, m.p. 138-139~C.
Exam~le 38 (a) To a suspension of K2CO3 (82.88 g, 0.6 mol) in CH3CN (300 ml) was added 3,5-dihydroxybenzoic acid (4.62 g, 0.03 mol), followed 10 minutes later by N-(2-chloroethyl)morpholine hydrochloride (18.42 g, 0.099 mol). The reaction mixture was refluxed overnight, cooled, filtered and the filtrate was concentrated in vacuo. The oily residue was purified by column chromatography on silica gel eluting with acetone, followed by W096/28448 PCT~S96J0310~

Kugelrohr distillation at > 195~C and 0.2 mm Hg .o afford 7.45 g of 4-mor~holinvlethvl 3,5-di-~2-(4-mor~holinvl)etho~ lbenzoate.
(b) A mixture of 4-morpholinylethyl 3,5-di-[2-(4-morpholinyl)ethoxy]benzoate (2.0 g, 4 mmol), 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamlde (0.45 g, 2 mmol), NaOCH3 (0.23 g, 4 mmol) and ethanol (50 ml) was refluxed for 96 hours.
The reaction was incomplete so an additional equivalent of the benzoate and NaOCH3 were added and the mixture was reluxed for 48 hours. The reaction mixture was stripped to dryness, and the residue was treated with water and acidified with acetic acid. The mixture was cooled and the product was isolated by filtration and dried at 90~C to af~ord 0 61 g (54%) of 1-cYclo~entYl-3-ethvl-~-r3,5-dir~-~4-mor~holinvl)etho~vl~henYll~vra~olo~3,--dl~vrimidin-4-one, m.p. 182-183~C.

Exam~le 39 To a suspension of 1-cyclopentyl-3-ethyl-5-[2-hydroxy-3-(2-propenyl)phenyl]pyrazolo[3,4-d]pyrimidin-4-one (1 0 g) in acetic acid (15 ml) was added sulfuric acid (15 m') while cooling in an ice bath The reaction mixture was Jarmed to room temperature and stirred overnight The reaction mixture was poured into iceiwate~, a precipitate formed which was collected by filtration and washed with water. The product was purified by recrystallization from ether, followed by column chromatography on silica gel eluting with 25% EtOAc/hexane to afford 0.5 g of 1-cvclo~entYl-3-ethvl-6-~2-methvl-2,3-dihvdrobenzorblfuran-5-vll~yrazolo~3,4-dl~yrimidin-4-one, m.p. 164-165~C.
Exam~le 40 (a) 3-(Ethcxycarbonylmethoxy)benzaldehyde (9.55 g, 45.91 mmol) was dissolved ~n ethanol (75 ml) and water '25 ml) and then ~OH
(3.02 g) was added. The reaction mixture was stirred at room temperature until the reaction was complete and then the product was collec~ed by filtration and dried to afford, as a white 3~

W 096/28448 PCTnUS96/03100 powder, 3.78 g of the ~otassium salt of 3-(carboxvmethoxv)benzaldehvde.
(b) The potassium salt of 3-(carboxymethoxy)benzaldehyde was dissolved in water and treated with 9N HMO3. A precipitate formed which was collected by filtration, washed with water and dried at 75~C under high vacuum to afford 1.66 g of 3-(carboxvmethoxY) .benzaldehvde .
( c ) 3-(Carboxymethox,v)benzaldehyde (1.63 g, 9.05 mmol) was dissolved in p-dioxane (20 ml) and cooled in an ice bath and then N,N~-carbonyldiimidazole (1.9 g) was added in one portion. The reaction mixture was stirred for 30 minutes, then morpholine (0.8 ml) was added and the mixture was warmed to room temperature and stirred until the reaction was complete. The solvent was removed in vacuo, the residue was partitioned between CHC13 (100 ml) and 2N HCl (75 ml), the layers were separated, and the aqueous layer was extracted with CHC13 (2 x 75 ml). The organic layers were combined, dried over MgSO4 and stripped to afford an oil which was combined with the product from a similar experimental run and purified by column chromatography on silica gel eluting with chloroform to afford 2.1 g of 3 - r 4 -mor~holinvlcarbonvlmethoxvlbenzaldehvde.
(d) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (1.87 g), 3-[4-morpholinylcarbonylmethoxy]benzaldehyde (2.1 g, 8.43 mmol) and xylenes (20 ml) was heated at 160~C for about 2 days. The solvent was removed, then methanol was added to the residue and the product was collected by filtration.
Additional product was obtained from the filtrates and the product frac~ions were pooled and recrystallized from CH3CN/CHC13 to afford 1 - c v c 1 o ~ e n t Y 1 - ~ - e t h v 1 - 5 - r 3 - ~ 4 -mor~holinvlcarbonylmethoxv)~henvll ~yrazolo~3.4-dl~vrimidin-~-one, m.p. 212-213~C.
Exam~le 41 (a) CA 022ll729 l997-07-29 W O 96/28448 YCTnUS96J03100 A mixture of 3-hydroxybenzaldehyde (5.17 g, 42.33 mmol), K2CO3 (58.5 g) and CH3CN (100 ml) was stirred at room temperature for 15 minutes, then dibromoethane (18.3 ml) was added. The reaction mixture was stirred at room temperature for 30 minutes, then at reflux for 3-4 hours. Additlonal dibromoethane was added and then the reaction mixture was refluxed overnight. The reaction mixture was cooled, filtered, and the filtrate was stripped to afford an oil. The oil was di~solved in ether (300 ml), washed with 5N NaOH (2 x 75 ml) and the ether layer was dried over MgSO4 and stripped. The residue was purified by column chromatography on silica gel eluting with 10% ethyl acetate/hexane to afford 5.23 g of 3-~2-bromoethoxv)benzaldehYde.

(b) A mixture of 3-(2-bromoethoxy)benzaldehyde (3.gl g, 17.07 mmol), K2C03 (3.1 g), thiomorpholine (1.9 ml) and DMF ( 30 ml) was warmed on a steambath overnight. Additional K2CO3 (0.7 g) and thiomorpholine (1.0 ml) were added and the reaction mixture was warmed on a steam bath overnight. The reaction mixture was cooled to room temperature, filtered and the filtrate was stripped to afford an amber oil. The oil was combined with the product from a similar experimental run and purified by column chromatography on silica gel eluting with EtOAc (100%) tO afford, as an oil, 3 (4-thiomor~holinvl)e~ho:~vlbenzaldehvde.
( c ) A mixture of 3-[2-(4-thiomorpholinyl)ethoxy]benzaldehyde (3.2 g, 12.75 mmol), 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (2.55 g) and xylenes (20 ml) was heated at 160~C
overnight. The reaction mixture was cooled in an ice bath, and then the solvent was removed to afford an oil which crystallized on standing. The product was treated with hot MeOH/Et2O, the mixture was cooled, and the product was collected by filtration and washed with ether tO afford 0.51 g of desired product. The filtrate was concentrated in vacuo to afford 5.0 g of the 6,7-dihydro derivative which was dissolved in xylenes (25 ml), treated with palladium on carbon and heated at 110~C for 3 hours.

W 096128448 PCTrUS96/03100 Additional palladiurn on carbon (1.5 g) was added and heating was continued for 2 hours. The mixture was filtered through CELITE(g) and the filtrate was stripped. The residue was treated with methanol and the product was collected by filtration and combined with the 0.51 g of product obtained above and the product obtained from a similar experimental run. The combined product fractions were recrystallized from EtOAc, washed with ether and dried at 100~C under high vacuum to afford 1-cvclo~entvl-3-ethvl-6-~3-~2-(4-thiomor~holinvl)ethoxvl~henvll ~vrazolor3,4-dl~vrimidin-4-one.
Exam~le 42 (a) To a mixture of 3-hydroxybenzonitrile (4.76 g, 0.04 mol), K2CO3 (16.6 g, 0.12 mol) and DMF (100 ml) under argon was added 4-chloromethylpyridine hydrochloride (6.56 g, 0.04 mol). The reaction mixture was stirred at room temperature for about two days, the solvent was evaporated and the residue was partitioned between water and CH~C12. The organic layer was washed with 2N
aqueous NaOH (1 x 100 rnl ), brine, then was dried over MgSO4. The solvent was removed in vacuo to afford, as an amber solid, 9.0 g of 3-(4-~vridinvlmethoxv)benzonitrile.

(b) A mixture of 3-(4-pyridinylmethoxy)benzor.itrile (2.5 g, 0.012 mol) in 75% formic acid ~35 ml) was treated with raney nickel (2 g) and heated to reflux for 4 hours. The reaction mixture was filtered through SUPE~CELL(~), the filtrate was brought to a pH of 8-9 with 5N NaOH, extracted with EtOAc (3 x 150 ml) and the combined organic layers were dried over MgSO4, filtered and stripped. The residue was purified by column chromatography on silica gel eluting with EtOAc (100%) to afford 0.94 g (37~,) of 3-(4-~vridinvlmethoxv) benzaldehvde.
(c ) A mixture of 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (2.7 g, 0.124 mol), 3-(4-pyridinylmethoxy)benzaldehyde (3.95 g, 0.0185 mol) and xylenes (100 ml) was refluxed overnight.
Additional carboxamide (1 g) was added and the mixture was WO 96/28448 PCTnUS96103100 refluxed for another 2 days. 10~ palladium on carbon (1 g) was added and the mixture was refluxed for another 3 hours. The catalyst was removed by filtration, the filtrate was concentrated in vacuo and the solid residue was collected ~y filtration.
Additional product ~as obtained by concentration of the mother li~uors and the combined product fractions were recrystallized from ethyl acetate to afford 1.66 g of 1-cvclo~entv'-3-ethYl-6-r3-~4-~vridinvlmethoxvl~)henvl1 ~vrazolo~3,4-dl~vrimidin-4-one, m.p. 230-232~C.
Exam~le 43 (a) A mixture of 3-hydroxybenzaldehyde (3.66 g, 0.03 mol), K2CO3 (12.43 g, 0.09 mol), and CH3CN (100 ml) was s_irred ~t room temperature for 1i2 hour, then N-methvl-2-chloromerhvlpiperidine hydrochloride ~5.49 g, 0.03 mol) was added. The reaction mixture was stirred until the reaction was complete, then ~he solvent was removed in vacuo and the residue was partitioned between CHCl3 and water. The aqueous layer was extracted with CHCl3 '_ x 100 ml) and the combined organic layers were concentrated in vacuo to afford 3-(1-methvi-3-he.Yahvdroaze~invloxy)ben7aldehvde.
(b) A mixture of 3-(1-methyl-3-hexahydroazepinyloxy) benzaldehyde (0.79 g, 3.4 mol), 1-cyciopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (0.5 g, 2.2 mmol), methanesulfonic acid (0.25 ml) and ~ylenes (25 ml) was refluxed overnigr.r. The solvent was stripped, the residue was dissolveà in CH2Cl2 and purified by column chromatography on silica gel eluting with ether, then acetone, then 0.5% Et3N/acetone to afford 0.43 g (45%) of _ cvclo~entv~-3-ethvl-6-- r3- (1-methYl-3-hexahvdroaze~invloxv)~h ~vrazolo~3,4-dl~vrimidin-4-one, m.p. 1~5-196~C.
Exam~le 44 To a mixture of 1-cyc~opentyl-3-ethyl-6-[3-[4-pyridinylmerhox~jphenyl]pyrazolo[3,4-c pvrimidin-4-one (1.1 g) in acetic aci~ (100 ml)iwater (50 ml) w_s added Pt2G (200 mgi. The mixture was hydrogenated at 50 psi with heating (variac set at 40) for four hours. The catalyst was removed by ~i'tration, the filtrate was ccncentrated and the residue was part-~ioned between =

W 096/28448 PCTrUS96/03100 NH40H and ethyl acetate. The organic layer was separated, .~ashed with brine, dried over MgSO4, filtered and concentrated. The residue was purified by column chromatography on silica gel-eluting with ethyl acetate, followed by preparative thin layer chromatography eluting with ethyl acetate to afford, after recrystallization from EtOAc, 64 mg of 1-cvclo~entvl-3-ethvl-5-(3-hvdroxv~henYl)~vrazolor3,4-dl~vrimidin-4-one, m.p. 275-278~C
(dec.).
Exam~le 45 (a) To a stirred solution of 3-hydroxybenzaldehyde (8 g, 65 mmol), 1-methyl-4-piperidinol (7.5 g, 65 mmol), triphenylphosphine (13.1 g, 65 mmol) and THF (100 ml) was added diethylazodicarboxylate (11.4 g, 65 mmol) in THF (20 ml) over a 35 minute period. The reaction mixture was stirred in an ice bath for 3 hours, then at room temperature for 5 days. The reaction mixture was concentrated in vacuo, and partitioned between CHCl3 (300 ml) and 3N HCl ~300 ml). The aqueous layer was concentrated in vacuo, the residue was treated with 10% K2CO3 and extracted with CHCl3 (2 x 100 ml). The solvent was removed in vacuo to afford 7.4 g of crude 3-!1-methvl-4-~i~eridinvloxY)benzaldehYde.

(b) . mixture of 3-(1-methyl-4-piperidinyloxy)ben_aldehyde (7.4 ~ , 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carbo~amide (2 g) and ,.-ylenes (200 ml) was refluxed for 31 hours and then was stirre~ at room temperature for several days. The solven~ was removec in vacuo, and the residue was purified by column chromatcgraphy on silica gel eluting with ether (100%) t~ 10%
methan~i/ether to afford, after recrystallization from isopropanol, ~.3 g of 1-cvclo~entvl 3-ethvl-6-~3-'1-methvl-4-~i~eric nvlo ~)~henYll~vrazolo ~3,4-dlPvrimidin-4-one 1/4 hvdrate Exam~le 46 (a) To a stirred solution of ',4-difluorobenzonitrile (~5 g, 0.18 mc:! n p-dioxane ( 50 ml) in an ice-bath was added scdium ethoxide (15 g, 0.22 mol) over 45 minutes. The reaction mixture was stirred as such for 2 hours, then at room temperature for 18 hours. The solvent was concentrated in vacuo and the residue was partitioned between water (200 ml) and CH2C12 (400 ml) and acidified with acetic acid. The organic layer was separated, dried over MgS04 and concentrated in vacuo to afford, as a yellow oil, 26.7 g of a mixture of 2-ethoxv-4-fluorobenzonitrile and 4-ethoxv-2-fluorobenzonitrile~
(b) To a mixture of the benzonitriles from Example 46 (a) (26.5 g, 0.16 mol), imidazole (11.5 g, 0.17 mol), and p-dioxane (150 ml) cooled in an ice bath was added NaH (6.8 g, 60%
dispersion in mineral oil) over a 30 minute period. The reaction mixture was stirred for 1 hour as such, then at room temperature for 24 hours, followed by standing at room temperature for 24 hours. The solvent was removed in vacuo, the residue was partitioned between CH2C12 (2 x 300 ml) and water (100 ml). The CH2C12 extracts were combined, concentrated in vacuo and the residue was purified by column chromatography on silica eluting with ether (100%) to 10% methanol/ether to afford 10.1 g of 4 imidazolvl)-2-ethoxv benzonitrile, m.p. 134-136~C.

( c ) A mixture of 1-cyciopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide (1.5 g, 6.3 mmol), 4- (1-imidazolyl) -2-ethoxybenzonitrile (1.5 g, 7 mmol), NaH (0.84 g, 21 mmol, 60%
dispersion in mineral oil! and p-dioxane (75 ml) was heated on a steam bath for 12 hours, then was stirred at room temperature overnight. The reaction m-xture was acidified with acetic acid, concentrated in vacuo, and water was added to the residue. A gummy solid formed which was collected, washed with water, dried and purified by column chromatography on silica gel eluting with ether (100%) to 15% methanol/ether to afford, after recrystallization from acetonitrile, 0.78 g ~36%) of 1-cvcloT~entvl-3-ethvl-6-~4-(1-imida7olvl!-2-ethoYvT~henv~lT~yrazolo~3,4-dlT~vrimidin-4-one, m.p.
204-206~C.

W 096128448 PCTrUS96/03100 Exam~le 47 Following a procedure similar to that described in Example 1 (c), but substituting 1-tert-butyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide for 1-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carboxamide and 2,4,6-trimethylbenzaldehyde for 2-propoxybenzaldehyde, it is contemplated that there can be prepared l-tert-butvl-3-ethvl-6-r2,4,6-trimethvl~henvll~vrazolor3,4-dl~vrimidin-4-one.
Exam~le 48 Following procedures similar to those described in Examples 1 (b) and 1 (c), but substituting 1-cyclopentyl-3-phenylmethyl-5-amino-lH-pyrazole-4-carbonitrile for l-cyclopentyl-3-ethyl-5-amino-lH-pyrazole-4-carbonitrile in part 1 (b), it is contemplated that there can be prepared:
(a) l-Cvclo~entvl-3-~henvlmethvl-5-amino-lH-~vrazole-4-carboxamide.
(b) l-Cvclo~entvl-3-~henvlmethvl-6-(2-~ro~oxv~henvl)~vrazolo r3,4-dl~vrimidin-4-one.

sioloaical Test ~esults In standard biological test procedures, the compounds of Formula I have been found to possess c-GMP-PDE V (formerly named as c-GMP-PDE I) inhibitory activity and are thus useful in the treatment of heart failure and hypertension. The compounds of Formula I, in combination with nitrates, have also been found to be useful in reversing or reducing nitrate-inauced tolerance and thus would be useful in the treatment of angina pectoris, congestive heart disease and myocardial infarction.
Multiple isozymic forms of cyclic nucleotide phosphodiesterase (PDE) have been identified in mammalian cells.
These isozymes hydrolyze cyclic adenosine monophosphate (cAMP) and/or cyclic guanosine monophosphate (cGMP) to the presumably biologically inactive 5~-nucleotide phosphates. Elevation of W O 96/28448 PCTrUS96103100 intracellular CGMP in vascular smooth muscle triggers a cascade of events that leads to a reduction in muscle tone ~Jhile elevations in renal tubule cell cGMP stimulates natriuresis and diuresis.
Vascular smooth musc-le and renal cells contain a phosphodiesterase isozyme that has a low Km (1 ~M) for the hydrolysis of cGMP. This isozyme has been referred to as the cGMP-PDE c- cGMP-PDE V
(formerly named as cGMP-PDE I since it eluted ~-om an anion-exchange sepharose resin in the first peak of PDE activity at a sodium acetate concentration between 150-200 mM). ~hus inhibition of the cGMP-PDE isozyme is a viable subcellular mechanism by which increases in cGMP can produce a reduction in total peripheral resistance and a stimulation of natriuresis and ~iuresi~. The development of cGMP-PDE inhibitors represents an a~proach for the discovery of agents useful f~r treating hear- failure and hypertension. For example, compounds having ,_~h inhibitory potency for the cGMP-PDE are expected to lower klocd pressure and induce natriuresis and diuresis.
The c-GMP-P]~E V inhibitory activity of representative compounds of the invention was demonstrated by -he following procedure.
The cGMP-PDE, and other PDE isozymes were ~solated from cardiovascular tissues (heart and aorta) of various animal species and man by anion-exchange and affinity chromatography as described by Silver et al., Sec. Messeng Phos. 13:13-~-, 1991; PDE
activity, n the presence and absence of tes~ _~mpounds was determined essentially as described by Thompson ~t al., Adv.
Cyclic Mucleotide Res. 10:69-92. To determine the potency and selectivity of compounds as PDE inhibitors, compounds are screened for their effect on cyclic nucleotide hydrolysis a~ 10 ~M. If 2 50% inhibition of PDE activity is observed, an ICso value (concentration of cornpound causing 50% reduction ir, PDE activity) and corresponding 95% confidence intervals are generated. The ICso values are calculated from concentration-response curves as described by Tallarida and Murray, Manual of ?harmacologic Calculations with Computer Programs, Procedure 8, Graded Dose-response, pp. 14-19, Springer-Verlag, New York, 1981.

W 096/28448 PCT~US96103100 The following table summarizes the results obtained from the testing of representative compounds of the invention.

Percent Inhibition at Given ~M or ICsO (nM) Exam~le No. cGMP-PDE V
l(c) 7/3 4 5.8 6 1.6 7 51% (10 ~M) or 20% (1 ~M) 8(a) 410/430*
8(b) 70% (1 ~M) or 32% (0.1 ~M) 9(b) 4.9 85% (10 ~lM) or 15% (1 ~LM) ll(c) 2700/4500*
12 (b) 74% (1 ~M) or 30% (0.1 ~M) 13(b) 107 16 68% (10 ~M) or 19% (1 ~M) or 780 nM

WO 96128448 P~TmS961D31~D

Percent Inhibition at Given ~M or ICso (nM) Example No. cGMP-PDE V
17(c) 14% (0.1 ~M) or 19% (1 ~M) or 39% (10 ~M) 18(b) 370 l9 (b ) 73 20( b ) 9 4 22 ( b ) 14 0 23(c) 540 24(C) 130 25 (b) 14/51*
26(c) 28% (1 ~M) 27(c) 73% (1 ~M) or 21% (0.1 ~M) 28 40~ M) 29(b) 7.4/8.4*
53% (1 ~M) or 9% (0.1 ~M) 31 61% (1 ~M) or 31% (0.1 ~M) 32 47% (1 ~M) or 23% (0.1 ~M) 33 56% (1 ~M) or 21% (0.1 ~M) 34 (b) 56% (0.1 ~M) or 28% (0.01 ~M) 35(b) 58% (0.1 ~M) or 13% (0.01 ~M) 36 0% (0.1 ~M) or 4% (1 ~M) 37(b) 73% (1 ~M) or 31% (0.1 ~M) 38(b) 63% (0.1 ~M) or 11% (0.01 ~M) 39 65% (0.1 ~M) or 24% (0.01 ~M) 40 (d) 74% (1 ~M) or 47% (0.1 ~M) 41(c) 56% (1 ~M) or 46% (0.1 ~M) 42(c) 56% (0.1 ~M) or 25% (0.01 ~M) 43(b) 75% (1 ~M) or 41% (0.1 ~M) 44 56% (1 ~M) or 29% (0.1 ~M) 46(c) 26% (0.1 ~M) or 76% (1 ~M) or 90%
(10 ~M) or 18 nM
*The numbers represent ICso (nM) values for separate experimentai runs.

W 096/28448 PCTrUS96103100 The antihypertensive activity of representative compounds of the invention was demonstrated by the following procedure.
Spontaneously hypertensive rats (SHR) were anesthetized with sodium pentobarbital (50 mg/kg, ip) and instrumented with catheters positioned in the inferior vena cava and abdominal aorta for administration of drug and recording of arterial pressure and heart rate, respectively. After a 2 day recovery from surgery, three baseline blood pressure measurements were made at 5 min intervals in conscious SHR. Compounds to be tested or vehicle were then administered intravenously in a dose-dependent manner (0.3-10 mg baseikg) while arterial pressure was recorded continuously on a polygraph. The mean arterial pressure response was measured 5 minutes after the administration of each dose of the test compound and the next dose given in a cumulative dose fashion. The response to each dose of the test compound was calculated as the difference from the mean of the three baseline measurements.
The foliowing table summarizes the results obtained from the testing of representative compounds of the invention.
SHR iv % change in mean arteriai pressure Example ~o. at Given mg/kg or ED~ (mg/kg) l(c) -5% (1 mg/kg) 3 -7% (1 mg/kg) 4 -13% (10 mg/kg) -8% (1 mgikg) 6 -1% (10 mg/kg) 8(a) 5.7 or -35% (10 mgikg) or -20% (3 mg/kg) or -81% (30 mg/kg, po) 9(b) -19% (10 mg/kg) 13(b) 9.5 or -58% (30 mg/kg, po) or -19% (3 mg/kg) or -14% ~1 mg/kg) or -11% (0.3 mg/kg) 19(b) 12.5 or -19% (10 mg/kg) 21 -1% (10 mg/kg) 22(b) 17.9 or -18% (10 mg/kg) 24(c) 12.7 or -21% (10 mg/kg) or -13% (3 mg/kg) 25(b) 4.5 or -38% (10 mg/kg) or -27% (3 mg/kg) or -18% (1 mg/kg) or -18% (10 mg/kg, po) W O 96128448 PCTnU~96)03~00 The activity of representative compounds of the invention in reversing or reducing nitrate-induced tolerance was demonstrated by the Eollowing procedure:
Spontaneously hypertensive rats (17-25 weeks of age) were made nitroglycerin tolerant by repeated administration of high doses of nitroglycerin (100 mg/kg, s.c., 3 times/day for 3 consecutive days). To confirm tolerance challenge doses of nitroglycerin were administered intravenously at doses ranging from 1-300 ~g/kg and the maximum change in mean arterial pressure (MAP) for each dose was recorded. Groups of tolerant rats were pretreated with the compounds of the invention (tolerant pretreated group) or with vehicle (0.05 N NaOH) (tolerant vehicle pretreated ~roup) intravenously 5-10 minutes prior to administration of challenge doses of nitroglycerin. The administration of challenge doses of nitroglycerin to non-tolerant rats (the non-tolerant group) caused a dose-dependent decrease in MAP of between 10 t~ 40 mm Hg, The administration of challenge doses of nitroglycerin to the tolerant vehicle pretreated group resulted in a significant reduction of the hypotensive response.
The administration of' challenge doses of nitroglycerin to tolerant rats which were pre~reated with the compounds of the invention (tolerant pretreated group) resulted in varying degrees of restoration of the hypotensive response. The area under the dose-MAP curve was calculated for the non-tolerant group and for the tolerant vehicle pretreated group and the tolerant pretreated group. The percent reversal of nitrate-induced tolerance was calculated as -ollows:

Percent Reversal = (Auctol-pretreated - AUCtol-veh)/(~UCnontol -AUCtol-veh) X 100 wherein: AUCnontol = the area under the dose-MAP curve for the non- tolera,.~ group.
AUCtol-veh = the area under the dose-MAP curve for the tolera,.t vehicle pretreated group.
AUCtcl-pretreated = the area under the dose-MAP curve for the tolera~.t pretreated group.

W 096/28448 PCTrUS96/03100 A percent reversal of 100% or greater reflects complete reversal of nitrate-induced tolerance, whereas a percent reversal of 0%
indicates that no reversal of nitrate-induced tolerance occurred.
The following table summarizes the results obtained from the testing of representative compounds of the invention.
Percent(%) Reversal of ExampleDose (mg/kq)Nitroqlycerin-induced Tolerance 6 1.0 49 8(a) 0.3 5 13(b) 0.3 58 The compounds of the invention can be prepared for pharmaceutical use by conventional pharmaceutical procedures that are well known in the arti that is, by formulating a pharmaceutical composition which comprises compounds of the invention or their pharmaceutically acceptable salts together with one or more physiologically acceptable carriers, adjuvants, diluents or vehicles, for oral administration in solid or liquid form, parenteral administration, topical administration or aerosol inhalation administration, and the like.
Solid compositions for oral administration include compressed tablets, pills, powders and granules. In such solid compositions, the active compound is admixed with at least one inert diluent such as starch, calcium carbonate, sucrose or lactcse. These compositions may also contain additional subs~ances other than inert diluents, e.g., lubricating agents, such as magnesium stearate, talc and the like.
Liquid compositions for oral administration include pharmaceutically acceptable emulsions, solutions, suspensions, syrups and elixirs containing inert diluents commonly used in the art, such as water and liquid paraffin. Besides inert diluents such compositions may also contain adjuvants, such as wetting and suspending agents, and sweetening, flavoring, perfuming and preserving agents. According to the invention, the compounds for oral administration also include capsules of absorbable material, W096/28448 ~C~lUS~6~D310D

such as gelatin, containing said active component with or without the addition of diluents or excipients.
Preparations according to the invention for parenteral administration inc].ude sterile aqueous, aqueous-organic, and organic solutions, suspensions and emulsions. Examples of organic solvents or suspending media are propylene glycol, polyethylene glycol, vegetable oils such as olive oil and injectable organic esters such as ethyl oleate. These compositions can also contain adjuvants such as stabilizing, preserving, wetting, emulsifying and dispersing agents.
Preparations according to the invention for topical administration or aerosol inhalation administration include dissolving or susp~nding a compound of the invention in a pharmaceutically acceptable vehicle such as water, aqueous alcohol, glycol, oil solution or oil-water emulsion, and the like.
If desired, the compounds of the invention can further be incorporated into slow release or targeted delivery systems such as polymer matrices, liposomes, and microspheres.
The percentage of active component in such compositions may be varied so that a suitable dosage is obtained. The dosage administered to a particular patient is variable depending upon the clinician~s judgment using as criteria: The route of administration, the duration of treatment, the size and physical condition of the patient, the potency of the active component and the patient's response thereto. An effective dosage amount of the active component can thus readily be determined by the clinician after a consideration of all criteria and using his best judgment on the patient~s behalf.

Claims (24)

We claim:

1. A compound of the formula:

wherein:
R1 is tert-butyl, or cyclopentyl;
R3 is lower-alkyl, or phenyl-lower-alkyl; and R6 is phenyl, or phenyl substituted by from one to three, the same or different, substituents selected from the group consisting of lower-alkoxy, lower-alkyl, hydroxy, 1-imidazolyl, lower-alkenyloxy, dilower-alkylamino-lower-alkoxy, 4-morpholinyl-lower-alkoxy, lower-alkoxycarbonyl-lower-alkoxy, carboxylower-alkoxy, trifluoromethyl, 1-piperidinyl-lower-alkoxy, 1-pyrrolidinyl-lower-alkoxy, nitro, halo, amino, -(CH2)2O-, lower-alkylsulfonylamino, lower-alkoxy-lower-alkoxy, lower-alkenyl, dilower-alkylamino, -OCH(CH3)CH2-, 4-morpholinylcarbonyl-lower-alkoxy, 4-thiomorpholinyl-lower-alkoxy, pyridinyl-lower-alkoxy, 1-lower-alkyl-3-hexahydroazepinyloxy, and 1-lower-alkyl-4-piperidinyl oxy; or a pharmaceutically acceptable acid-addition salt and/or hydrate thereof.

2. A compound according to Claim 1 wherein R1 is cyclopentyl;
and R3 is lower-alkyl.

3. A compound according to Claim 2 wherein R3 is methyl or ethyl.

4. A compound according to Claim 3 wherein R6 is phenyl, or phenyl substituted by from one to two, the same or different, substituents selected from the group consisting of lower-alkoxy, lower-alkyl, hydroxy, 1-imidazo1yl, lower-alkenyloxy, dilower-alkylamino-lower-alkoxy, 4-morpholinyl-lower-alkoxy, lower-alkoxycarbonyl-lower-alkoxy, carboxylower-alkoxy, trifluoromethyl, 1-piperidinyl-lower-alkoxy, 1-pyrrolidinyl-lower-alkoxy, nitro, halo, amino, -(CH2)2O-, lower-alkylsulfonylamino, lower-alkoxy-lower-alkoxy, lower-alkenyl, dilower-alkylamino, -OCH(CH3)CH2-, 4-morpholinylcarbonyl-lower-alkoxy, 4-thiomorpholinyl-lower-alkoxy, pyridinyl-lower-alkoxy, 1-lower-alkyl-3-hexahydroazepinyloxy, and 1-lower-alkyl-4-piperidinyloxy.

5. A compound according to Claim 4 wherein R6 is phenyl, or phenyl substituted by from one to two, the same or different, substituents selected from the group consisting of methoxy, ethoxy, propoxy, methyl, hydroxy, 1-imidazolyl, CH2=CHCH2O-, 2-(dimethylamino)ethoxy, 3-(dimethylamino)propoxy, 2-(4-morpholinyl)ethoxy, 3-(4-morpholinyl)propoxy, ethoxycarbonylmethoxy, carboxymethoxy, trifluoromethyl, 2-(1-piperidinyl)ethoxy, 2-(1-pyrrolidinyl)ethoxy, nitro, chloro, amino, -(CH2)2O-, methylsulfonylamino, 2-(methoxy)ethoxy, CH2=CH2CH2-, diethylamino, -OCH(CH3)CH2-, 4-morpholinyl-carbonylmethoxy, 2-(4-thiomorpholinyl)ethoxy, 4-pyridinylmethoxy, 1-methyl-3-hexahydroazepinyloxy, and 1-methyl-4-piperidinyloxy.

6. A compound according to Claim 5 selected from the group consisting of:
1- cyclopentyl-3-ethyl-6-(2-propoxyphenyl)pyrazolo[3,4-d]
pyrimindin-4-one, 1-cyclopentyl-3-ethyl-6-[4-(1-imidazolyl)phenyl]pyrazolo [3,4-d]pyrimindin-4-one, 1-cyclopentyl-3-ethyl-6-[3-(2-(4-morpholinyl)ethoxy) phenyl]pyrazolo[3,4-d]pyrimindin-4-one, 1-cyclopentyl-3-ethyl-6-[2-ethoxy-4-(1-imidazolyl)phenyl]
pyrazolo[3,4-d]pyrimindin-4-one, and 1-cyclopentyl-3-ethyl-6-[2-(CH2=CHCH2O)phenyl]pyrazolo [3,4-d] pyrimindin-4-one.

7. A pharmaceutical composition which comprises a compound according to claim 1 together with a pharmaceutically acceptable carrier, adjuvant, diluent, or vehicle.

8. A pharmaceutical composition which comprises a compound according to claim 2 together with a pharmaceutically acceptable carrier, adjuvant, diluent, or vehicle.

9. A pharmaceutical composition which comprises a compound according to claim 3 together with a pharmaceutically acceptable carrier, adjuvant, diluent, or vehicle.

10. A pharmaceutical composition which comprises a compound according to claim 4 together with a pharmaceutically acceptable carrier, adjuvant, diluent, or vehicle.

11. A pharmaceutical composition which comprises a compound according to claim 5 together with a pharmaceutically acceptable carrier, adjuvant, diluent, or vehicle.

12. A pharmaceutical composition which comprises a compound according to claim 6 together with a pharmaceutically acceptable carrier, adjuvant, diluent, or vehicle.

13. A method for effecting cGMP-phosphodiesterase inhibition in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 1.

14. A method for effecting cGMP-phosphodiesterase inhibition in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 2.

15. A method for effecting cGMP-phosphodiesterase inhibition in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 3.

16. A method for effecting cGMP-phosphodiesterase inhibition in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 4.

17. A method for effecting cGMP-phosphodiesterase inhibition in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 5.

18. A method for effecting cGMP-phosphodiesterase inhibition in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 6.

19. A method for treating heart failure and/or hypertension in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 1.

20. A method for treating heart failure and/or hypertension in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 2.

21. A method for treating heart failure and/or hypertension in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 3.

22. A method for treating heart failure and/or hypertension in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 4.

23. A method for treating heart failure and/or hypertension in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 5.

24. A method for treating heart failure and/or hypertension in a mammalian organism which comprises administering to said organism an effective amount of a compound according to claim 6.